Prostate cancer markers

ABSTRACT

The present invention relates to a composition comprising a plurality of cDNAs which are differentially expressed in prostate cancer and which may be used in their entirety or in part as to diagnose, to stage to treat or to monitor the treatment of a subject with prostate cancer.

[0001] This application is a continuation of U.S. application Ser. No. 09/919,172, filed Jul. 30, 2001, which further claims the benefit of U.S. Provisional Application Ser. No. 60/222,469, filed Jul. 28, 2000.

FIELD OF THE INVENTION

[0002] The present invention relates to a composition comprising a plurality of cDNAs which are differentially expressed in prostate cancer and which may be used entirely or in part to diagnose, to stage, to treat, or to monitor the progression or treatment of prostate cancer.

BACKGROUND OF THE INVENTION

[0003] Array technology can provide a simple way to explore the expression of a single polymorphic gene or the expression profile of a large number of related or unrelated genes. When the expression of a single gene is examined, arrays are employed to detect the expression of a specific gene or its variants. When an expression profile is examined, arrays provide a platform for examining which genes are tissue specific, carrying out housekeeping functions, parts of a signaling cascade, or specifically related to a particular genetic predisposition, condition, disease, or disorder.

[0004] The potential application of gene expression profiling is particularly relevant to improving diagnosis, prognosis, and treatment of disease. For example, both the levels and sequences expressed in tissues from subjects with prostate cancer may be compared with the levels and sequences expressed in normal tissue.

[0005] Prostate cancer is a common malignancy in men over the age of 50, and the incidence increases with age. In the US, there are approximately 132,000 newly diagnosed cases of prostate cancer and more than 33,000 deaths from the disorder each year.

[0006] Once cancer cells arise in the prostate, they are stimulated by testosterone to a more rapid growth. Thus, removal of the testes can indirectly reduce both rapid growth and metastasis of the cancer. Over 95 percent of prostatic cancers are adenocarcinomas which originate in the prostatic acini. The remaining 5 percent are divided between squamous cell and transitional cell carcinomas, both of which arise in the prostatic ducts or other parts of the prostate gland.

[0007] As with most cancers, prostate cancer develops through a multistage progression ultimately resulting in an aggressive, metastatic phenotype. The initial step in tumor progression involves the hyperproliferation of normal luminal and/or basal epithelial cells that become hyperplastic and evolve into early-stage tumors. The early-stage tumors are localized in the prostate but eventually may metastasize, particularly to the bone, brain or lung. About 80% of these tumors remain responsive to androgen treatment, an important hormone controlling the growth of prostate epithelial cells. However, in its most advanced state, cancer growth becomes androgen-independent and there is currently no known treatment for this condition.

[0008] A primary diagnostic marker for prostate cancer is prostate specific antigen (PSA). PSA is a tissue-specific serine protease almost exclusively produced by prostatic epithelial cells. The quantity of PSA correlates with the number and volume of the prostatic epithelial cells, and consequently, the levels of PSA are an excellent indicator of abnormal prostate growth. Men with prostate cancer exhibit an early linear increase in PSA levels followed by an exponential increase prior to diagnosis. However, since PSA levels are also influenced by factors such as inflammation, androgen and other growth factors, some scientists maintain that changes in PSA levels are not useful in detecting individual cases of prostate cancer.

[0009] Current areas of cancer research provide additional prospects for markers as well as potential therapeutic targets for prostate cancer. Several growth factors have been shown to play a critical role in tumor development, growth, and progression. The growth factors Epidermal Growth Factor (EGF), Fibroblast Growth Factor (FGF), and Tumor Growth Factor alpha (TGFα) are important in the growth of normal as well as hyperproliferative prostate epithelial cells, particularly at early stages of tumor development and progression, and affect signaling pathways in these cells in various ways (Lin J et al. (1999) Cancer Res. 59:2891-2897; Putz T et al. (1999) Cancer Res 59:227-233). The TGF-β family of growth factors are generally expressed at increased levels in human cancers and the high expression levels in many cases correlates with advanced stages of malignancy and poor survival (Gold L I (1999) Crit Rev Oncog 10:303-360). Finally, there are human cell lines representing both the androgen-dependent stage of prostate cancer (LNCap) as well as the androgen-independent, hornone refractory stage of the disease (PC3 and DU-145) that have proved useful in studying gene expression patterns associated with the progression of prostate cancer, and the effects of cell treatments on these expressed genes (Chung T D (1999) Prostate 15:199-207).

[0010] The present invention provides for a composition comprising a plurality of cDNAs for use in detecting changes in expression of genes encoding proteins that are associated with prostate cancer. Such a composition can be employed for the diagnosis, prognosis or treatment of prostate cancer and related disorders correlated with differential gene expression. The present invention satisfies a need in the art in that it provides a set of differentially expressed genes which may be used entirely or in part to diagnose, to stage, to treat, or to monitor the progression or treatment of a subject with prostate cancer.

SUMMARY

[0011] The present invention provides a composition comprising a plurality of cDNAs and their complements which are differentially expressed in prostate adenocarcinomas and which are selected from SEQ ID NOs:1-1-3, 5, 6, 8, 10-15, 17-19, 21, 23-28, 30, 32, 34-36, 38, 40, 42-45, 47-50, 52, 53, 55, 56, 58-65, 67, 68, 70-73, 75, 76, 78-86, 88-90, 92-97, 99-101 as presented in the Sequence Listing. In one embodiment, each cDNA is differentially regulated in metastatic versus non-metastatic tissue samples, SEQ ID NOs:1-3, 5, 6, 8, 10-15, 17-19, 21, 23-28, 30, 32, 34-36, 38, 40, 42-45, 47-50, 52, 53, 55, 56, 58-65, 67, 68, 70-73, 75; in another embodiment, each cDNA is differentially regulated at all stages of the disease, SEQ ID NOs:76, 78-86, 88-90, 92-97, 99-101. In one aspect, the composition is immobilized on a substrate. In another aspect, the composition is used to diagnose the presence and stage of prostate cancer in a subject. The invention also provides proteins encoded by the cDNAs and which are selected from SEQ ID NOs:4, 7, 9, 16, 20, 22, 29, 31, 33, 37, 39, 41, 46, 51, 54, 57, 66, 69, 74, 77, 87, 91, 98 as presented in the Sequence Listing.

[0012] The invention also provides a high throughput method to detect differential expression of one or more of the cDNAs of the composition. The method comprises hybridizing the substrate comprising the composition with the nucleic acids of a sample, thereby forming one or more hybridization complexes, detecting the hybridization complexes, and comparing the hybridization complexes with those of a standard, wherein differences in the size and signal intensity of each hybridization complex indicates differential expression of nucleic acids in the sample. In one aspect, the sample is from a subject with prostate cancer and differential expression determines an early, mid, and late stage of the disorder.

[0013] The invention further provides a high throughput method of screening a library or a plurality of molecules or compounds to identify a ligand. The method comprises combining the substrate comprising the composition with a library or a plurality of molecules or compounds under conditions to allow specific binding and detecting specific binding, thereby identifying a ligand. The library or a plurality of molecules or compounds are selected from DNA molecules, RNA molecules, peptide nucleic acid molecules, mimetics, peptides, transcription factors, repressors, and other regulatory proteins.

[0014] The invention still further provides an isolated cDNA encoding the protein comprising the amino acid sequence of SEQ ID NO:37. The invention also provides an isolated cDNA comprising SEQ ID NO:36 as presented in the Sequence Listing. The invention also provides a vector comprising the cDNA, a host cell comprising the vector, and a method for producing a protein comprising culturing the host cell under conditions for the expression of a protein and recovering the protein from the host cell culture. The invention additionally provides a method for purifying a ligand, the method comprising combining a cDNA of the invention with a sample under conditions which allow specific binding, recovering the bound cDNA, and separating the cDNA from the ligand, thereby obtaining purified ligand.

[0015] The present invention provides a purified protein encoded and produced by a cDNA of the invention. The invention also provides a high-throughput method for using a protein to screen a library or a plurality of molecules or compounds to identify a ligand. The method comprises combining the protein or a portion thereof with the library or a plurality of molecules or compounds under conditions to allow specific binding and detecting specific binding, thereby identifying a ligand which specifically binds the protein. A library or a plurality of molecules or compounds are selected from DNA molecules, RNA molecules, peptide nucleic acid molecules, mimetics, peptides, proteins, agonists, antagonists, antibodies or their fragments, immunoglobulins, inhibitors, drug compounds, and pharmaceutical agents. The invention further provides for using a protein to purify a ligand. The method comprises combining the protein or a portion thereof with a sample under conditions to allow specific binding, recovering the bound protein, and separating the protein from the ligand, thereby obtaining purified ligand. The invention still further provides a pharmaceutical composition comprising the protein. The invention yet still further provides a method for using the protein to produce an antibody. The method comprises immunizing an animal with the protein or an antigenically-effective epitope under conditions to elicit an antibody response, isolating animal antibodies, and screening the isolated antibodies with the protein to identify an antibody which specifically binds the protein. The invention yet still further provides a method for using the protein to purify antibodies which bind specifically to the protein.

DESCRIPTION OF THE SEQUENCE LISTING AND TABLES

[0016] A portion of the disclosure of this patent document contains material that is subject to copyright protection. The copyright owner has no objection to the facsimile reproduction by anyone of the patent document or the patent disclosure, as it appears in the Patent and Trademark Office patent file or records, but otherwise reserves all copyright rights whatsoever.

[0017] The Sequence Listing is a compilation of cDNAs obtained by sequencing and extension of clone inserts. Each sequence is identified by a sequence identification number (SEQ ID NO) and by the template number (TEMPLATE ID) from which it was obtained.

[0018] Table 1 shows the differential expression of cDNAs of the present invention in metastatic versus non-metastatic prostate adenocarcinoma. Column 1 shows the Clone ID of each sequence represented on a microarray. Columns 2-6 show differential expression in adenocarcinomas derived from prostate tissue relative to primary prostate epithelium Differential expression values are presented as log2(normal tissue/adenocarcinoma). Negative values represent an increase in expression. Column 7 shows the t-test statistic used to evaluate markers specific to metastatic versus non-metastatic prostate adenocarcinoma.

[0019] Table 2 shows the differential expression of cDNAs of the present invention in prostate adenocarcinoma versus normal prostate. Column 1 shows the Clone ID of each sequence represented on a microarray. Columns 2-6 show differential expression in adenocarcinomas derived from prostate tissue relative to primary prostate epithelium Differential expression values are presented as log2(normal tissue/adenocarcinoma). Negative values represent an increase in expression.

[0020] Table 3 shows the region within a gene template of each cDNA encompassed by a clone identified in Tables 1 and 2. Columns 1 and 2 show the SEQ ID NO: and Template ID, respectively. Column 3 shows the Clone ID and columns 4 and 5 show the first residue (Start) and last residue (Stop) encompassed by the clone on the template.

[0021] Table 4 lists the functional annotation of the cDNAs of the present invention. Columns 1 and 2 show the SEQ ID NO and Template ID, respectively. Columns 3, 4, and 5 show the GenBank hit (GI Number), probability score (E-value), and functional annotation, respectivly, as determined by BLAST analysis (version 1.4 using default parameters; Altschul (1993) J Mol Evol 36: 290-300; Altschul et al. (1990) J Mol Biol 215:403-410) of the cDNA against GenBank (release 117; National Center for Biotechnology Information (NCBI), Bethesda Md.).

[0022] Table 5 shows Pfam annotations of the cDNAs of the present invention. Columns 1 and 2 show the SEQ ID NO and Template ID, respectively. Columns 3, 4, and 5 show the first residue (Start), last residue (Stop), and reading frame, respectively, for the segment of the cDNA identified by Pfam analysis. Columns 6, 7, and 8 show the PFAM Hit, PFAM Annotation, and E-value, respectively, corresponding to the polypeptide domain of the protein or encoded by the cDNA segment.

[0023] Table 6 shows signal peptide and transiembrane regions predicted within the cDNAs of the present invention. Columns 1 and 2 show the SEQ ID NO and Template ID, respectively. Columns 3, 4, and 5 show the first residue (Start), last residue (Stop), and reading frame, respectively, for a segment of the cDNA, and column 6 identifies the polypeptide encoded by the segment as either a signal peptide (SP) or transmembrane (TM) domain.

DESCRIPTION OF THE INVENTION

[0024] Definitions

[0025] “Array” refers to an ordered arrangement of at least two cDNAs on a substrate. At least one of the cDNAs represents a control or standard sequence, and the other, a cDNA of diagnostic interest. The arrangement of from about two to about 40,000 cDNAs on the substrate assures that the size and signal intensity of each labeled hybridization complex formied between a cDNA and a sample nucleic acid is individually distinguishable.

[0026] The “complement” of a nucleic acid molecule of the Sequence Listing refers to a cDNA which is completely complementary over the full length of the sequence and which will hybridize to the nucleic acid molecule under conditions of high stringency.

[0027] A “composition” comprises at least two sequences selected from the Sequence Listing. “cDNA” refers to a chain of nucleotides, an isolated polynucleotide, nucleic acid molecule, or any fragment or complement thereof. It may have originated recombinantly or synthetically, be double-stranded or single-stranded, coding and/or noncoding, an exon with or without an intron from a genomic DNA molecule, and purified or combined with carbohydrate, lipids, protein or inorganic elements or substances. Preferably, the cDNA is from about 4000 to about 5000 nucleotides.

[0028] The phrase “cDNA encoding a protein” refers to a nucleic acid sequence that closely aligns with sequences which encode conserved regions, motifs or domains that were identified by employing analyses well known in the art. These analyses include BLAST (Basic Local Alignment Search Tool; Altschul (1993) J Mol Evol 36: 290-300; Altschul et al. (1990) J Mol Biol 215:403-410) which provides identity within the conserved region. Brenner et al. (1998; Proc Natl Acad Sci 95:6073-6078) who analyzed BLAST for its ability to identify structural homologs by sequence identity found 30% identity is a reliable threshold for sequence alignments of at least 150 residues and 40% is a reasonable threshold for alignments of at least 70 residues (Brenner et al., page 6076, column 2).

[0029] “Derivative” refers to a cDNA or a protein that has been subjected to a chemical modification. Derivatization of a cDNA can involve substitution of a nontraditional base such as queosine or of an analog such as hypoxanthine. These substitutions are well known in the art. Derivatization of a protein involves the replacement of a hydrogen by an acetyl, acyl, alkyl, amino, formyl, or morpholino group. Derivative molecules retain the biological activities of the naturally occurring molecules but may confer advantages such as longer lifespan or enhanced activity.

[0030] “Differential expression” refers to an increased, upregulated or present, or decreased, downregulated or absent, gene expression as detected by the absence, presence, or at least two-fold changes in the amount of transcribed messenger RNA or translated protein in a sample.

[0031] “Disorder” refers to conditions, diseases or syndromes associated with prostate cancer.

[0032] “Fragment” refers to a chain of consecutive nucleotides from about 200 to about 700 base pairs in length. Fragments may be used in PCR or hybridization technologies to identify related nucleic acid molecules and in binding assays to screen for a ligand. Nucleic acids and their ligands identified in this manner are useful as therapeutics to regulate replication, transcription or translation.

[0033] A “hybridization complex” is formed between a cDNA and a nucleic acid of a sample when the purines of one molecule hydrogen bond with the pyrimidines of the complementary molecule, e.g., 5′-A-G-T-C-3′ base pairs with 3′-T-C-A-G-5′. The degree of complementarity and the use of nucleotide analogs affect the efficiency and stringency of hybridization reactions.

[0034] “Ligand” refers to any agent, molecule, or compound which will bind specifically to a complementary site on a cDNA molecule or polynucleotide, or to an epitope or a protein. Such ligands stabilize or modulate the activity of polynucleotides or proteins and may be composed of inorganic or organic substances including nucleic acids, proteins, carbohydrates, fats, and lipids.

[0035] “Oligonucleotide” refers a single stranded molecule from about 18 to about 60 nucleotides in length which may be used in hybridization or amplification technologies or in regulation of replication, transcription or translation. Substantially equivalent terms are amplimer, primer, and oligomer.

[0036] “Portion” refers to any part of a protein used for any purpose; but especially, to an epitope for the screening of ligands or for the production of antibodies.

[0037] “Post-translational modification” of a protein can involve lipidation, glycosylation, phosphorylation, acetylation, racemization, proteolytic cleavage, and the like. These processes may occur synthetically or biochemically. Biochemical modifications will vary by cellular location, cell type, pH, enzymatic milieu, and the like.

[0038] “Probe” refers to a cDNA that hybridizes to at least one nucleic acid molecule in a sample. Where targets are single stranded, probes are complementary single strands. Probes can be labeled with reporter molecules for use in hybridization reactions including Southern, northern, in situ, dot blot, array, and like technologies or in screening assays.

[0039] “Protein” refers to a polypeptide or any portion thereof. A “portion” of a protein retains at least one biological or antigenic characteristic of a native protein. An “oligopeptide” is an amino acid sequence from about five residues to about 15 residues that is used as part of a fusion protein to produce an antibody.

[0040] “Purified” refers to any molecule or compound that is separated from its natural environment and is from about 60% free to about 90% free from other components with which it is naturally associated.

[0041] “Sample” is used in its broadest sense as containing nucleic acids, proteins, antibodies, and the like. A sample may comprise a bodily fluid; the soluble fraction of a cell preparation, or an aliquot of media in which cells were grown; a chromosome, an organelle, or membrane isolated or extracted from a cell; genomic DNA, RNA, or cDNA in solution or bound to a substrate; a cell; a tissue; a tissue print; a fingerprint, buccal cells, skin, or hair; and the like.

[0042] “Specific binding” refers to a special and precise interaction between two molecules which is dependent upon their structure, particularly their molecular side groups. For example, the intercalation of a regulatory protein into the major groove of a DNA molecule, the hydrogen bonding along the backbone between two single stranded nucleic acids, or the binding between an epitope of a protein and an agonist, antagonist, or antibody.

[0043] “Similarity” as applied to sequences, refers to the quantification (usually percentage) of nucleotide or residue matches between at least two sequences aligned using a standardized algorithm such as Smith-Waterman alignment (Smith and Waterman (1981) J Mol Biol 147:195-197) or BLAST2 (Altschul et al. (1997) Nucleic Acids Res 25:3389-3402). BLAST2 may be used in a standardized and reproducible way to insert gaps in one of the sequences in order to optimize alignment and to achieve a more meaningful comparison between them

[0044] “Substrate” refers to any rigid or semi-rigid support to which cDNAs or proteins are bound and includes membranes, filters, chips, slides, wafers, fibers, magnetic or nonmagnetic beads, gels, capillaries or other tubing, plates, polymers, and microparticles with a variety of surface forms including wells, trenches, pins, channels and pores.

[0045] “Variant” refers to molecules that are recognized variations of a cDNA or a protein encoded by the cDNA. Splice variants may be determined by BLAST score, wherein the score is at least 100, and most preferably at least 400. Allelic variants have a high percent identity to the cDNAs and may differ by about three bases per hundred bases. “Single nucleotide polymorphism” (SNP) refers to a change in a single base as a result of a substitution, insertion or deletion. The change may be conservative (purine for purine) or non-conservative (purine to pyrimidine) and may or may not result in a change in an encoded amino acid.

THE INVENTION

[0046] The present invention provides for a composition comprising a plurality of cDNAs or their complements, SEQ ID NOs:1-3, 5, 6, 8, 10-15, 17-19, 21, 23-28, 30, 32, 34-36, 38, 40, 42-45, 47-50, 52, 53, 55, 56, 58-65, 67, 68, 70-73, 75, 76, 78-86, 88-90, 92-97, 99-101, which may be used on a substrate to diagnose, to stage, to treat or to monitor the progression or treatment of prostate cancer. These cDNAs represent known and novel genes differentially expressed in cells from non-metastatic and metastatic prostate tumors. The composition may be used in its entirety or in part, as subsets of cDNAs differentially regulated between non-metastatic and metastatic prostate cancer, SEQ ID NOs:1-3, 5, 6, 8, 10-15, 17-19, 21, 23-28, 30, 32, 34-36, 38, 40, 42-45, 47-50, 52, 53, 55, 56, 58-65, 67, 68, 70-73, 75, or of cDNAs differentially regulated at all stages of prostate cancer, SEQ ID NOs:76, 78-86, 88-90, 92-97, 99-101. SEQ ID NOs:24, 36, 47, 60, 82, 88, 89, 92, 93, and 95 represent novel cDNAs associated with prostate cancer. Since the novel cDNAs were identified solely by their differential expression, it is not essential to know a priori the name, structure, or function of the gene or it's encoded protein. The usefulness of the novel cDNAs exist in their immediate value as diagnostics for prostate cancer.

[0047] Table 1 shows the differential expression of cDNAs of the present invention in metastatic versus non-metastatic prostate adenocarcinoma. Column 1 shows the Clone ID of each sequence represented on a microarray. Columns 2-6 show the differential expression in adenocarcinomas derived from prostate tissue relative to primary prostate epithelium Differential expression values are presented as log 2 of the absolute expression in normal prostate tissue ÷the absolute expression in prostate adenocarcinoma. Negative values represent an increase in expression. Column 7 shows the t-test statistic used to evaluate markers specific to metastatic versus non-metastatic prostate adenocarcinoma. All of the cDNAs in Table 1 show significant differential regulation in metastatic cancer relative to non-metastatic cancer. Further, expression profiles between the metastatic cancer lines show a high degree of correlation (>0.48), as do the expression profiles between the non-metastatic lines (0.64). However, the expression profiles between the metastatic and non-metastatic lines show significantly less correlation (<0.3).

[0048] Table 2 shows the differential expression of cDNAs of the present invention in prostate adenocarcinoma versus normal prostate. Column 1 shows the Clone ID of each sequence represented on a microarray. Columns 2-6 show differential expression in adenocarcinomas derived from prostate tissue relative to primary prostate epithelium Differential expression values are presented as log2 (normal tissue ÷adenocarcinoma). Negative values represent an increase in expression. The expression profile for the cDNAs identified in Table 2 show high correlation between all tumor lines (>0.5).

[0049] SEQ ID NO:36 is a novel sequence differentially regulated between metastatic and non-metastatic prostate tumors. SEQ ID NO:36 encodes SEQ ID NO:37 which is 193 amino acids in length.

[0050] The cDNAs of the invention define a differential expression pattern against which to compare the expression pattern of biopsied and/or in vitro treated tissues. Experimentally, differential expression of the cDNAs can be evaluated by methods including, but not limited to, differential display by spatial immobilization or by gel electrophoresis, genome mismatch scanning, representational discriminate analysis, clustering, transcript imaging and array technologies. These methods may be used alone or in combination.

[0051] The composition may be arranged on a substrate and hybridized with tumor tissues from subjects to identify those sequences which are differentially expressed in both prostate cancer and tumors derived from other tissues. This allows identification of those sequences of highest diagnostic and potential therapeutic value. In one embodiment, an additional set of cDNAs, such as cDNAs encoding signaling molecules, are arranged on the substrate with the composition. Such combinations may be useful in the elucidation of pathways which are affected in a particular cancer or to identify new, coexpressed, candidate, therapeutic molecules.

[0052] In another embodiment, the composition can be used for large scale genetic or gene expression analysis of a large number of novel, nucleic acid molecules. These samples are prepared by methods well known in the art and are from mammalian cells or tissues which are in a certain stage of development; have been treated with a known molecule or compound, such as a cytokine, growth factor, a drug, and the like; or have been extracted or biopsied from a mammal with a known or unknown condition, disorder, or disease before or after treatment. The sample nucleic acid molecules are hybridized to the composition for the purpose of defining a novel gene profile associated with that developmental stage, treatment, or disorder.

[0053] cDNAs and Their Uses

[0054] cDNAs can be prepared by a variety of synthetic or enzymatic methods well known in the art. cDNAs can be synthesized, in whole or in part, using chemical methods well known in the art (Caruthers et al. (1980) Nucleic Acids Symp. Ser. (7):215-233). Alternatively, cDNAs can be produced enzymatically or recombinantly, by in vitro or in vivo transcription.

[0055] Nucleotide analogs can be incorporated into cDNAs by methods well known in the art. The only requirement is that the incorporated analog must base pair with native purines or pyrimidines. For example, 2,6-diaminopurine can substitute for adenine and form stronger bonds with thymidine than those between adenine and thymidine. A weaker pair is formed when hypoxanthine is substituted for guanine and base pairs with cytosine. Additionally, cDNAs can include nucleotides that have been derivatized chemically or enzymatically.

[0056] cDNAs can be synthesized on a substrate. Synthesis on the surface of a substrate may be accomplished using a chemical coupling procedure and a piezoelectric printing apparatus as described by Baldeschweiler et al. (PCT publication WO95/251116). Alternatively, the cDNAs can be synthesized on a substrate surface using a self-addressable electronic device that controls when reagents are added as described by Heller et al. (U.S. Pat. No. 5,605,662). cDNAs can be synthesized directly on a substrate by sequentially dispensing reagents for their synthesis on the substrate surface or by dispensing preformed DNA fragments to the substrate surface. Typical dispensers include a micropipette delivering solution to the substrate with a robotic system to control the position of the micropipette with respect to the substrate. There can be a multiplicity of dispensers so that reagents can be delivered to the reaction regions efficiently.

[0057] cDNAs can be immobilized on a substrate by covalent means such as by chemical bonding procedures or UV irradiation. In one method, a cDNA is bound to a glass surface which has been modified to contain epoxide or aldehyde groups. In another method, a cDNA is placed on a polylysine coated surface and UV cross-linked to it as described by Shalon et al. (WO95/35505). In yet another method, a cDNA is actively transported from a solution to a given position on a substrate by electrical means (Heller, supra). cDNAs do not have to be directly bound to the substrate, but rather can be bound to the substrate through a linker group. The linker groups are typically about 6 to 50 atoms long to provide exposure of the attached cDNA. Preferred linker groups include ethylene glycol oligomers, dianines, diacids and the like. Reactive groups on the substrate surface react with a terminal group of the linker to bind the linker to the substrate. The other terminus of the linker is then bound to the cDNA. Alternatively, polynucleotides, plasmids or cells can be arranged on a filter. In the latter case, cells are lysed, proteins and cellular components degraded, and the DNA is coupled to the filter by UV cross-linking.

[0058] The cDNAs may be used for a variety of purposes. For example, the composition of the invention may be used on an array. The array, in turn, can be used in high-throughput methods for detecting a related polynucleotide in a sample, screening a plurality of molecules or compounds to identify a ligand, diagnosing prostate cancer, or inhibiting or inactivating a therapeutically relevant gene related to the cDNA.

[0059] When the cDNAs of the invention are employed on a microarray, the cDNAs are arranged in an ordered fashion so that each cDNA is present at a specified location. Because the cDNAs are at specified locations on the substrate, the hybridization patterns and intensities, which together create a unique expression profile, can be interpreted in terms of expression levels of particular genes and can be correlated with a particular metabolic process, condition, disorder, disease, stage of disease, or treatment. Hybridization

[0060] The cDNAs or fragments or complements thereof may be used in various hybridization technologies. The cDNAs may be labeled using a variety of reporter molecules by either PCR, recombinant, or enzymatic techniques. For example, a commercially available vector containing the cDNA is transcribed in the presence of an appropriate polymerase, such as T7 or SP6 polymerase, and at least one labeled nucleotide. Commercial kits are available for labeling and cleanup of such cDNAs. Radioactive (Amersham Pharmacia Biotech (APB), Piscataway N.J.), fluorescent (Operon Technologies, Alameda Calif.), and chemiluminescent labeling (Promega, Madison Wis.) are well known in the art.

[0061] A cDNA may represent the complete coding region of an mRNA or be designed or derived from unique regions of the mRNA or genomic molecule, an intron, a 3′untranslated region, or from a conserved motif. The cDNA is at least 18 contiguous nucleotides in length and is usually single stranded. Such a cDNA may be used under hybridization conditions that allow binding only to an identical sequence, a naturally occurring molecule encoding the same protein, or an allelic variant. Discovery of related human and mammalian sequences may also be accomplished using a pool of degenerate cDNAs and appropriate hybridization conditions. Generally, a cDNA for use in Southern or northern hybridizations may be from about 400 to about 6000 nucleotides long. Such cDNAs have high binding specificity in solution-based or substrate-based hybridizations. An oligonucleotide, a fragment of the cDNA, may be used to detect a polynucleotide in a sample using PCR.

[0062] The stringency of hybridization is determined by G+C content of the cDNA, salt concentration, and temperature. In particular, stringency is increased by reducing the concentration of salt or raising the hybridization temperature. In solutions used for some membrane based hybridizations, addition of an organic solvent such as formamide allows the reaction to occur at a lower temperature. Hybridization may be performed with buffers, such as 5× saline sodium citrate (SSC) with 1% sodium dodecyl sulfate (SDS) at 60° C., that permit the formation of a hybridization complex between nucleic acid sequences that contain some mismatches. Subsequent washes are performed with buffers such as 0.2×SSC with 0.1% SDS at either 45° C. (medium stringency) or 65°-68° C. (high stringency). At high stringency, hybridization complexes will remain stable only where the nucleic acid molecules are completely complementary. In some membrane-based hybridizations, preferably 35% or most preferably 50%, formamide may be added to the hybridization solution to reduce the temperature at which hybridization is performed. Background signals may be reduced by the use of detergents such as Sarkosyl or Triton X-100 (Sigma Aldrich, St. Louis Mo.) and a blocking agent such as denatured salmon sperm DNA. Selection of components and conditions for hybridization are well known to those skilled in the art and are reviewed in Ausubel et al. (1997, Short Protocols in Molecular Biology, John Wiley & Sons, New York N.Y., Units 2.8-2.11, 3.18-3.19 and 4-6-4.9).

[0063] Dot-blot, slot-blot, low density and high density arrays are prepared and analyzed using methods known in the art. cDNAs from about 18 consecutive nucleotides to about 5000 consecutive nucleotides in length are contemplated by the invention and used in array technologies. The preferred number of cDNAs on an array is at least about 100,000, a more preferred number is at least about 40,000, an even more preferred number is at least about 10,000, and a most preferred number is at least about 600 to about 800. The array may be used to monitor the expression level of large numbers of genes simultaneously and to identify genetic variants, mutations, and SNPs. Such information may be used to determine gene function; to understand the genetic basis of a disorder; to diagnose a disorder; and to develop and monitor the activities of therapeutic agents being used to control or cure a disorder. (See, e.g., U.S. Pat. No. 5,474,796; WO95/11995; WO95/35505; U.S. Pat. No. 5,605,662; and U.S. Pat. No. 5,958,342.)

[0064] Screening and Purification Assays

[0065] A cDNA may be used to screen a library or a plurality of molecules or compounds for a ligand which specifically binds the cDNA. Ligands may be DNA molecules, RNA molecules, peptide nucleic acid molecules, peptides, proteins such as transcription factors, promoters, enhancers, repressors, and other proteins that regulate replication, transcription, or translation of the polynucleotide in the biological system. The assay involves combining the cDNA or a fragment thereof with the molecules or compounds under conditions that allow specific binding and detecting the bound cDNA to identify at least one ligand that specifically binds the cDNA.

[0066] In one embodiment, the cDNA may be incubated with a library of isolated and purified molecules or compounds and binding activity determined by methods such as a gel-retardation assay (U.S. Pat. No. 6,010,849) or a reticulocyte lysate transcriptional assay. In another embodiment, the cDNA may be incubated with nuclear extracts from biopsied and/or cultured cells and tissues. Specific binding between the cDNA and a molecule or compound in the nuclear extract is initially determined by gel shift assay. Protein binding may be confirmed by raising antibodies against the protein and adding the antibodies to the gel-retardation assay where specific binding will cause a supershift in the assay.

[0067] In another embodiment, the cDNA may be used to purify a molecule or compound using affinity chromatography methods well known in the art. In one embodiment, the cDNA is chemically reacted with cyanogen bromide groups on a polymeric resin or gel. Then a sample is passed over and reacts with or binds to the cDNA. The molecule or compound which is bound to the cDNA may be released from the cDNA by increasing the salt concentration of the flow-through medium and collected.

[0068] The cDNA may be used to purify a ligand from a sample. A method for using a cDNA to purify a ligand would involve combining the cDNA or a fragment thereof with a sample under conditions to allow specific binding, recovering the bound cDNA, and using an appropriate agent to separate the cDNA from the purified ligand.

[0069] Protein Production and Uses

[0070] The full length cDNAs or fragment thereof may be used to produce purified proteins using recombinant DNA technologies described herein and taught in Ausubel et al. (supra; Units 16.1-16.62). One of the advantages of producing proteins by these procedures is the ability to obtain highly-enriched sources of the proteins thereby simplifying purification procedures.

[0071] The proteins may contain amino acid substitutions, deletions or insertions made on the basis of similarity in polarity, charge, solubility, hydrophobicity, hydrophilicity, and/or the amphipathic nature of the residues involved. Such substitutions may be conservative in nature when the substituted residue has structural or chemical properties similar to the original residue (e.g., replacement of leucine with isoleucine or valine) or they may be nonconservative when the replacement residue is radically different (e.g., a glycine replaced by a tryptophan). Computer programs included in LASERGENE software (DNASTAR, Madison Wis.), MACVECTOR software (Genetics Computer Group, Madison Wis.) and RasMol software (www.umass.edu/microbio/rasmol) may be used to help determine which and how many amino acid residues in a particular portion of the protein may be substituted, inserted, or deleted without abolishing biological or immunological activity.

[0072] Expression of Encoded Proteins

[0073] Expression of a particular cDNA may be accomplished by cloning the cDNA into a vector and transforming this vector into a host cell. The cloning vector used for the construction of cDNA libraries in the LIFESEQ databases may also be used for expression. Such vectors usually contain a promoter and a polylinker useful for cloning, priming, and transcription. An exemplary vector may also contain the promoter for β-galactosidase, an amino-terminal methionine and the subsequent seven amino acid residues of β-galactosidase. The vector may be transformed into competent E. coli cells. Induction of the isolated bacterial strain with isopropylthiogalactoside (IPTG) using standard methods will produce a fusion protein that contains an N terminal methionine, the first seven residues of β-galactosidase, about 15 residues of linker, and the protein encoded by the cDNA.

[0074] The cDNA may be shuttled into other vectors known to be useful for expression of protein in specific hosts. Oligonucleotides containing cloning sites and fragments of DNA sufficient to hybridize to stretches at both ends of the cDNA may be chemically synthesized by standard methods. These primers may then be used to amplify the desired fragments by PCR. The fragments may be digested with appropriate restriction enzymes under standard conditions and isolated using gel electrophoresis. Alternatively, similar fragments are produced by digestion of the cDNA with appropriate restriction enzymes and filled in with chemically synthesized oligonucleotides. Fragments of the coding sequence from more than one gene may be ligated together and expressed.

[0075] Signal sequences that dictate secretion of soluble proteins are particularly desirable as component parts of a recombinant sequence. For example, a chimeric protein may be expressed that includes one or more additional purification-facilitating domains. Such domains include, but are not limited to, metal-chelating domains that allow purification on immobilized metals, protein A domains that allow purification on immobilized immunoglobulin, and the domain utilized in the FLAGS extension/affinity purification system (Immunex, Seattle Wash.). The inclusion of a cleavable-linker sequence such as ENTEROKINASEMAX (Invitrogen, San Diego Calif.) between the protein and the purification domain may also be used to recover the protein.

[0076] Suitable host cells may include, but are not limited to, mammalian cells such as Chinese Hamster Ovary (CHO) and human 293 cells, insect cells such as Sf9 cells, plant cells such as Nicotiana tabacum, yeast cells such as Saccharomyces cerevisiae, and bacteria such as E. coli. For each of these cell systems, a useful vector may also include an origin of replication and one or two selectable markers to allow selection in bacteria as well as in a transformed eukaryotic host. Vectors for use in eukaryotic host cells may require the addition of 3′ poly(A) tail if the cDNA lacks poly(A).

[0077] Additionally, the vector may contain promoters or enhancers that increase gene expression. Many promoters are known and used in the art. Most promoters are host specific and exemplary promoters includes SV40 promoters for CHO cells; T7 promoters for bacterial hosts; viral promoters and enhancers for plant cells; and PGH promoters for yeast. Adenoviral vectors with the rous sarcoma virus enhancer or retroviral vectors with long terminal repeat promoters may be used to drive protein expression in mammalian cell lines. Once homogeneous cultures of recombinant cells are obtained, large quantities of secreted soluble protein may be recovered from the conditioned medium and analyzed using chromatographic methods well known in the art. An alternative method for the production of large amounts of secreted protein involves the transformation of mammalian embryos and the recovery of the recombinant protein from milk produced by transgenic cows, goats, sheep, and the like.

[0078] In addition to recombinant production, proteins or portions thereof may be produced manually, using solid-phase techniques (Stewart et al. (1969) Solid-Phase Peptide Synthesis, W H Freeman, San Francisco Calif.; Merrifield (1963) J Am Chem Soc 5:2149-2154), or using machines such as the ABI 431A peptide synthesizer (Applied Biosystems, Foster City Calif.). Proteins produced by any of the above methods may be used as pharmaceutical compositions to treat disorders associated with null or inadequate expression of the genomic sequence.

[0079] Screening and Purification Assays

[0080] A protein or a portion thereof encoded by the cDNA may be used to screen a library or a plurality of molecules or compounds for a ligand with specific binding affinity or to purify a molecule or compound from a sample. The protein or portion thereof employed in such screening may be free in solution, affixed to an abiotic or biotic substrate, or located intracellularly. For example, viable or fixed prokaryotic host cells that are stably transformed with recombinant nucleic acids that have expressed and positioned a protein on their cell surface can be used in screening assays. The cells are screened against a library or a plurality of ligands and the specificity of binding or formation of complexes between the expressed protein and the ligand may be measured. The ligands may be DNA, RNA, or PNA molecules, agonists, antagonists, antibodies, immunoglobulins, inhibitors, peptides, pharmaceutical agents, proteins, drugs, or any other test molecule or compound that specifically binds the protein. An exemplary assay involves combining the mammalian protein or a portion thereof with the molecules or compounds under conditions that allow specific binding and detecting the bound protein to identify at least one ligand that specifically binds the protein.

[0081] This invention also contemplates the use of competitive drug screening assays in which neutralizing antibodies capable of binding the protein specifically compete with a test compound capable of binding to the protein or oligopeptide or fragment thereof. One method for high throughput screening using very small assay volumes and very small amounts of test compound is described in U.S. Pat. No. 5,876,946. Molecules or compounds identified by screening may be used in a model system to evaluate their toxicity, diagnostic, or therapeutic potential.

[0082] The protein may be used to purify a ligand from a sample. A method for using a protein to purify a ligand would involve combining the protein or a portion thereof with a sample under conditions to allow specific binding, recovering the bound protein, and using an appropriate chaotropic agent to separate the protein from the purified ligand.

[0083] Production of Antibodies

[0084] A protein encoded by a cDNA of the invention may be used to produce specific antibodies. Antibodies may be produced using an oligopeptide or a portion of the protein with inherent immunological activity. Methods for producing antibodies include: 1) injecting an animal, usually goats, rabbits, or mice, with the protein, or an antigenically-effective portion or an oligopeptide thereof, to induce an immune response; 2) engineering hybridomas to produce monoclonal antibodies; 3) inducing in vivo production in the lymphocyte population; or 4) screening libraries of recombinant immunoglobulins. Recombinant immunoglobulins may be produced as taught in U.S. Pat. No. 4,816,567.

[0085] Antibodies produced using the proteins of the invention are useful for the diagnosis of prepathologic disorders as well as the diagnosis of chronic or acute diseases characterized by abnormalities in the expression, amount, or distribution of the protein. A variety of protocols for competitive binding or immunoradiometric assays using either polyclonal or monoclonal antibodies specific for proteins are well known in the art. Immunoassays typically involve the formation of complexes between a protein and its specific binding molecule or compound and the measurement of complex formation. Immunoassays may employ a two-site, monoclonal-based assay that utilizes monoclonal antibodies reactive to two noninterfering epitopes on a specific protein or a competitive binding assay (Pound (1998) Immunochemical Protocols, Humana Press, Totowa N.J.).

[0086] Immunoassay procedures may be used to quantify expression of the protein in cell cultures, in subjects with a particular disorder or in model animal systems under various conditions. Increased or decreased production of proteins as monitored by immunoassay may contribute to knowledge of the cellular activities associated with developmental pathways, engineered conditions or diseases, or treatment efficacy. The quantity of a given protein in a given tissue may be determined by performing immunoassays on freeze-thawed detergent extracts of biological samples and comparing the slope of the binding curves to binding curves generated by purified protein.

[0087] Labeling of Molecules for Assay

[0088] A wide variety of reporter molecules and conjugation techniques are known by those skilled in the art and may be used in various cDNA, polynucleotide, protein, peptide or antibody assays. Synthesis of labeled molecules may be achieved using commercial kits for incorporation of a labeled nucleotide such as ³²P-dCTP, Cy3-dCTP or Cy5-dCTP or amino acid such as ³⁵S-methionine. Polynucleotides, cDNAs, proteins, or antibodies may be directly labeled with a reporter molecule by chemical conjugation to amines, thiols and other groups present in the molecules using reagents such as BIODIPY or FITC (Molecular Probes, Eugene Oreg.).

[0089] The proteins and antibodies may be labeled for purposes of assay by joining them, either covalently or noncovalently, with a reporter molecule that provides for a detectable signal. A wide variety of labels and conjugation techniques are known and have been reported in the scientific and patent literature including, but not limited to U.S. Pat. Nos. 3,817,837; 3,850,752; 3,939,350; 3,996,345; 4,277,437; 4,275,149; and 4,366,241.

[0090] Diagnostics

[0091] The cDNAs, or fragments thereof, may be used to detect and quantify differential gene expression; absence, presence, or excess expression of mRNAs; or to monitor mRNA levels during therapeutic intervention in subjects with prostate-related disorders including prostate cancer. These cDNAs can also be utilized as markers of treatment efficacy against prostate cancer over a period ranging from several days to months. The diagnostic assay may use hybridization or amplification technology to compare gene expression in a biological sample from a patient to standard samples in order to detect altered gene expression. Qualitative or quantitative methods for this comparison are well known in the art.

[0092] For example, the cDNA may be labeled by standard methods and added to a biological sample from a patient under conditions for hybridization complex formation. After an incubation period, the sample is washed and the amount of label (or signal) associated with hybridization complexes is quantified and compared with a standard value. If the amount of label in the patient sample is significantly altered in comparison to the standard value, then the presence of the associated condition, disease or disorder is indicated.

[0093] In order to provide a basis for the diagnosis of a condition, disease or disorder associated with gene expression, a normal or standard expression profile is established. This may be accomplished by combining a biological sample taken from normal subjects, either animal or human, with a probe under conditions for hybridization or amplification. Standard hybridization may be quantified by comparing the values obtained using normal subjects with values from an experiment in which a known amount of a substantially purified target sequence is used. Standard values obtained in this manner may be compared with values obtained from samples from patients who are symptomatic for a particular condition, disease, or disorder. Deviation from standard values toward those associated with a particular condition is used to diagnose that condition.

[0094] Such assays may also be used to evaluate the efficacy of a particular therapeutic treatment regimen in animal studies and in clinical trial or to monitor the treatment of an individual patient. Once the presence of a condition is established and a treatment protocol is initiated, diagnostic assays may be repeated on a regular basis to determine if the level of expression in the patient begins to approximate that which is observed in a normal subject. The results obtained from successive assays may be used to show the efficacy of treatment over a period ranging from several days to months.

[0095] Gene Expression Profiles

[0096] A gene expression profile comprises a plurality of cDNAs and a plurality of detectable hybridization complexes, wherein each complex is formed by hybridization of one or more probes to one or more complementary sequences in a sample. The cDNA composition of the invention is used as elements on a microarray to analyze gene expression profiles. In one embodiment, the microarray is used to monitor the progression of prostate cancer. Researchers can assess and catalog the differences in gene expression between healthy and diseased tissues or cells. By analyzing changes in patterns of gene expression, prostate cancer can be diagnosed at earlier stages before the patient is symptomatic. The invention can be used to formulate a prognosis and to design a treatment regimen. The invention can also be used to monitor the efficacy of treatment. For treatments with known side effects, the microarray is employed to improve the treatment regimen. A dosage is established that causes a change in genetic expression patterns indicative of successful treatment. Expression patterns associated with the onset of undesirable side effects are avoided. This approach may be more sensitive and rapid than waiting for the patient to show inadequate improvement, or to manifest side effects, before altering the course of treatment.

[0097] In another embodiment, animal models which mimic a human disease can be used to characterize expression profiles associated with a particular condition, disorder or disease; or treatment of the condition, disorder or disease. Novel treatment regimens may be tested in these animal models using microarrays to establish and then follow expression profiles over time. In addition, microarrays may be used with cell cultures or tissues removed from animal models to rapidly screen large numbers of candidate drug molecules, looking for ones that produce an expression profile similar to those of known therapeutic drugs, with the expectation that molecules with the same expression profile will likely have similar therapeutic effects. Thus, the invention provides the means to rapidly determine the molecular mode of action of a drug.

[0098] Assays Using Antibodies

[0099] Antibodies directed against epitopes on a protein encoded by a cDNA of the invention may be used in assays to quantify the amount of protein found in a particular human cell. Such assays include methods utilizing the antibody and a label to detect expression level under normal or disease conditions. The antibodies may be used with or without modification, and labeled by joining them, either covalently or noncovalently, with a labeling moiety.

[0100] Protocols for detecting and measuring protein expression using either polyclonal or monoclonal antibodies are well known in the art. Examples include ELISA, RIA, and fluorescent activated cell sorting (FACS). Such immunoassays typically involve the formation of complexes between the protein and its specific antibody and the measurement of such complexes. These and other assays are described in Pound (supra). The method may employ a two-site, monoclonal-based immunoassay utilizing monoclonal antibodies reactive to two non-interfering epitopes, or a competitive binding assay. (See, e.g., Coligan et al. (1997) Current Protocols in Immunology, Wiley-Interscience, New York N.Y.; Pound, supra)

[0101] Therapeutics

[0102] The cDNAs and fragments thereof can be used in gene therapy. cDNAs can be delivered ex vivo to target cells, such as cells of bone marrow. Once stable integration and transcription and or translation are confirmed, the bone marrow may be reintroduced into the subject. Expression of the protein encoded by the cDNA may correct a cancer associated with mutation of a normal sequence, reduction or loss of an endogenous target protein, or overepression of an endogenous or mutant protein. Alternatively, cDNAs may be delivered in vivo using vectors such as retrovirus, adenovirus, adeno-associated virus, herpes simplex virus, and bacterial plasmids. Non-viral methods of gene delivery include cationic liposomes, polylysine conjugates, artificial viral envelopes, and direct injection of DNA (Anderson (1998) Nature 392:25-30; Dachs et al. (1997) Oncol Res 9:313-325; Chu et al. (1998) J Mol Med 76(3-4):184-192; Weiss et al. (1999) Cell Mol Life Sci 55(3):334-358; Agrawal (1996) Antisense Therapeutics, Humana Press, Totowa N.J.; and August et al. (1997) Gene Therapy (Advances in Pharmacology, Vol. 40), Academic Press, San Diego Calif.).

[0103] In addition, expression of a particular protein can be regulated through the specific binding of a fragment of a cDNA to a genomic sequence or an mRNA which encodes the protein or directs its transcription or translation. The cDNA can be modified or derivatized to any RNA-like or DNA-like material including peptide nucleic acids, branched nucleic acids, and the like. These sequences can be produced biologically by transforming an appropriate host cell with a vector containing the sequence of interest.

[0104] Molecules which regulate the activity of the cDNA or encoded protein are useful as therapeutics for prostate cancer. Such molecules include agonists which increase the expression or activity of the polynucleotide or encoded protein, respectively; or antagonists which decrease expression or activity of the polynucleotide or encoded protein, respectively. In one aspect, an antibody which specifically binds the protein may be used directly as an antagonist or indirectly as a delivery mechanism for bringing a pharmaceutical agent to cells or tissues which express the protein.

[0105] Additionally, any of the proteins, or their ligands, or complementary nucleic acid sequences may be administered as pharmaceutical compositions or in combination with other appropriate therapeutic agents. Selection of the appropriate agents for use in combination therapy may be made by one of ordinary skill in the art, according to conventional pharmaceutical principles. The combination of therapeutic agents may act synergistically to affect the treatment or prevention of the conditions and disorders associated with an immune response. Using this approach, one may be able to achieve therapeutic efficacy with lower dosages of each agent, thus reducing the potential for adverse side effects. Further, the therapeutic agents may be combined with pharmaceutically-acceptable carriers including excipients and auxiliaries which facilitate processing of the active compounds into preparations which can be used pharmaceutically. Further details on techniques for formulation and administration used by doctors and pharmacists may be found in the latest edition of Remington's Pharmaceutical Sciences (Maack Publishing, Easton Pa.).

[0106] Model Systems

[0107] Animal models may be used as bioassays where they exhibit a phenotypic response similar to that of humans and where exposure conditions are relevant to human exposures. Mammals are the most common models, and most infectious agent, cancer, drug, and toxicity studies are performed on rodents such as rats or nice because of low cost, availability, lifespan, reproductive potential, and abundant reference literature. Inbred and outbred rodent strains provide a convenient model for investigation of the physiological consequences of underexpression or overexpression of genes of interest and for the development of methods for diagnosis and treatment of diseases. A mammal inbred to overexpress a particular gene (for example, secreted in milk) may also serve as a convenient source of the protein expressed by that gene.

[0108] Transgenic Animal Models

[0109] Transgenic rodents that overexpress or underexpress a gene of interest may be inbred and used to model human diseases or to test therapeutic or toxic agents. (See, e.g., U.S. Pat. No. 5,175,383 and U.S. Pat. No. 5,767,337.) In some cases, the introduced gene may be activated at a specific time in a specific tissue type during fetal or postnatal development. Expression of the transgene is monitored by analysis of phenotype, of tissue-specific mRNA expression, or of serum and tissue protein levels in transgenic animals before, during, and after challenge with experimental drug therapies.

[0110] Embryonic Stem Cells

[0111] Embryonic (ES) stem cells isolated from rodent embryos retain the potential to form embryonic tissues. When ES cells such as the mouse 129/SvJ cell line are placed in a blastocyst from the C57BL/6 mouse strain, they resume normal development and contribute to tissues of the live-born animal. ES cells are preferred for use in the creation of experimental knockout and knockin animals. The method for this process is well known in the art and the steps are: the cDNA is introduced into a vector, the vector is transformed into ES cells, transformed cells are identified and microinjected into mouse cell blastocysts, blastocysts are surgically transferred to pseudopregnant dans. The resulting chimeric progeny are genotyped and bred to produce heterozygous or homozygous strains.

[0112] Knockout Analysis

[0113] In gene knockout analysis, a region of a gene is enzymatically modified to include a non-natural intervening sequence such as the neomycin phosphotransferase gene (neo; Capecchi (1989) Science 244:1288-1292). The modified gene is transformed into cultured ES cells and integrates into the endogenous genome by homologous recombination. The inserted sequence disrupts transcription and translation of the endogenous gene.

[0114] Knockin Analysis

[0115] ES cells can be used to create knockin humanized animals or transgenic animal models of human diseases. With knockin technology, a region of a human gene is injected into animal ES cells, and the human sequence integrates into the animal cell genome. Transgenic progeny or inbred lines are studied and treated with potential pharmaceutical agents to obtain information on the progression and treatment of the analogous human condition.

[0116] As described herein, the uses of the cDNAs, provided in the Sequence Listing of this application, and their encoded proteins are exemplary of known techniques and are not intended to reflect any limitation on their use in any technique that would be known to the person of average skill in the art. Furthermore, the cDNAs provided in this application may be used in molecular biology techniques that have not yet been developed, provided the new techniques rely on properties of nucleotide sequences that are currently known to the person of ordinary skill in the art, e.g., the triplet genetic code, specific base pair interactions, and the like. Likewise, reference to a method may include combining more than one method for obtaining or assembling full length cDNA sequences that will be known to those skilled in the art. It is also to be understood that this invention is not limited to the particular methodology, protocols, and reagents described, as these may vary. It is also understood that the terminology used herein is for the purpose of describing particular embodiments only, and is not intended to limit the scope of the present invention which will be limited only by the appended claims. The examples below are provided to illustrate the subject invention and are not included for the purpose of limiting the invention.

EXAMPLES

[0117] I Construction of cDNA Libraries

[0118] RNA was purchased from Clontech Laboratories (Palo Alto Calif.) or isolated from various tissues. Some tissues were homogenized and lysed in guanidinium isothiocyanate, while others were homogenized and lysed in phenol or in a suitable mixture of denaturants, such as TRIZOL reagent (Life Technologies, Rockville Md.). The resulting lysates were centrifuged over CsCl cushions or extracted with chloroform. RNA was precipitated with either isopropanol or ethanol and sodium acetate, or by other routine methods.

[0119] Phenol extraction and precipitation of RNA were repeated as necessary to increase RNA purity. In most cases, RNA was treated with DNase. For most libraries, poly(A) RNA was isolated using oligo d(T)-coupled paramagnetic particles (Promega), OLIGOTEX latex particles (Qiagen, Valencia Calif.), or an OLIGOTEX mRNA purification kit (Qiagen). Alternatively, poly(A) RNA was isolated directly from tissue lysates using other kits, including the POLY(A)PURE mRNA purification kit (Ambion, Austin Tex.).

[0120] In some cases, Stratagene (La Jolla Calif.) was provided with RNA and constructed the corresponding cDNA libraries. Otherwise, cDNA was synthesized and cDNA libraries were constructed with the UNIZAP vector system (Stratagene) or SUPERSCRIPT plasmid system (Life Technologies) using the recommended procedures or similar methods known in the art. (See Ausubel, supra, Units 5.1 through 6.6.) Reverse transcription was initiated using oligo d(T) or random primers. Synthetic oligonucleotide adapters were ligated to double stranded cDNA, and the cDNA was digested with the appropriate restriction enzyme or enzymes. For most libraries, the cDNA was size-selected (300-1000 bp) using SEPHACRYL S 1000, SEPHAROSE CL2B, or SEPHAROSE CL4B column chromatography (APB) or preparative agarose gel electrophoresis. cDNAs were ligated into compatible restriction enzyme sites of the polylinker of the PBLUESCRIPT phagemid (Stratagene), PSPORT1 plasmid (Life Technologies), or PINCY plasmid (Incyte Pharmaceuticals). Recombinant plasmids were transformed into XL1-BLUE, XL1-BLUEMRF, or SOLR competent E. coli cells (Stratagene) or DH5a, DH10B, or ELECTROMAX DH10B competent E. coli cells (Life Technologies).

[0121] In some cases, libraries were superinfected with a 5× excess of the helper phage, M13K07, according to the method of Vieira et al. (1987, Methods Enzymol. 153:3-11) and normalized or subtracted using a methodology adapted from Soares (1994, Proc Natl Acad Sci 91:9228-9232), Swaroop et al. (1991, Nucl Acids Res 19:1954), and Bonaldo et al. (1996, Genome Research 6:791-806). The modified Soares normalization procedure was utilized to reduce the repetitive cloning of highly expressed high abundance cDNAs while maintaining the overall sequence complexity of the library. Modification included significantly longer hybridization times which allowed for increased gene discovery rates by biasing the normalized libraries toward those infrequently expressed low-abundance cDNAs which are poorly represented in a standard transcript image (Soares et al., supra).

[0122] II Isolation and Sequencing of cDNA Clones

[0123] Plasmids were recovered from host cells by in vivo excision using the UNIZAP vector system (Stratagene) or by cell lysis. Plasmids were purified using one of the following: the Magic or WIZARD MINIPREPS DNA purification system (Promega); the AGTC MINIPREP purification kit (Edge BioSystems, Gaithersburg Md.); the QIAWELL 8, QIAWELL 8 Plus, or QIAWELL 8 Ultra plasmid purification systems, or the REAL PREP 96 plasmid purification kit (QIAGEN, Valencia Calif.). Following precipitation, plasmids were resuspended in 0.1 ml of distilled water and stored, with or without lyophilization, at 4° C.

[0124] Alternatively, plasmid DNA was amplified from host cell lysates using direct link PCR in a high-throughput format (Rao (1994) Anal Biochem 216:1-14). Host cell lysis and thermal cycling steps were carried out in a single reaction mixture. Samples were processed and stored in 384-well plates, and the concentration of amplified plasmid DNA was quantified fluorometrically using PICOGREEN dye (Molecular Probes) and a FLUOROSKAN II fluorescence scanner (Labsystems Oy, Helsinki, Finland).

[0125] cDNA sequencing reactions were processed using standard methods or high-throughput instrumentation such as the ABI CATALYST 800 thermal cycler (Applied Biosystems) or the DNA ENGINE thermal cycler (MJ Research, Watertown Mass.) in conjunction with the HYDRA microdispenser (Robbins Scientific, Sunnyvale Calif.) or the MICROLAB 2200 system (Hamilton, Reno Nev.). cDNA sequencing reactions were prepared using reagents provided by APB or supplied in ABI sequencing kits such as the ABI PRISM BIGDYE cycle sequencing kit (Applied Biosystems). Electrophoretic separation of cDNA sequencing reactions and detection of labeled cDNAs were carried out using the MEGABACE 1000 DNA sequencing system (APB); the ABI PRISM 373 or 377 sequencing systems (Applied Biosystems) in conjunction with standard ABI protocols and base calling software; or other sequence analysis systems known in the art. Reading frames within the cDNA sequences were identified using standard methods (reviewed in Ausubel, supra, Unit 7.7).

[0126] III Extension of cDNA Sequences

[0127] Nucleic acid sequences were extended using the cDNA clones and oligonucleotide primers. One primer was synthesized to initiate 5′ extension of the known fragment, and the other, to initiate 3′ extension of the known fragment. The initial primers were designed using OLIGO 4.06 software (National Biosciences), or another appropriate program, to be about 22 to 30 nucleotides in length, to have a GC content of about 50% or more, and to anneal to the target sequence at temperatures of about 68° C. to about 72° C. Any stretch of nucleotides which would result in hairpin structures and primer-primer dimerizations was avoided.

[0128] Selected human cDNA libraries were used to extend the sequence. If more than one extension was necessary or desired, additional or nested sets of primers were designed. Preferred libraries are ones that have been size-selected to include larger cDNAs. Also, random primed libraries are preferred because they will contain more sequences with the 5′ and upstream regions of genes. A randomly primed library is particularly useful if an oligo d(T) library does not yield a full-length cDNA.

[0129] High fidelity amplification was obtained by PCR using methods well known in the art. PCR was performed in 96-well plates using the DNA ENGINE thermal cycler (MJ Research). The reaction mix contained DNA template, 200 nmol of each primer, reaction buffer containing Mg²⁺, (NH₄)₂SO₄, and β-mercaptoethanol, Taq DNA polymerase (APB), ELONGASE enzyme (Life Technologies), and Pfu DNA polymerase (Stratagene), with the following parameters for primer pair PCI A and PCI B (Incyte Pharmaceuticals): Step 1: 94° C., 3 min; Step 2: 94° C., 15 sec; Step 3: 60° C., 1 min; Step 4: 68° C., 2 min; Step 5: Steps 2, 3, and 4 repeated 20 times; Step 6: 68° C., 5 min; Step 7: storage at 4° C. In the alternative, the parameters for primer pair T7 and SK+ (Stratagene) were as follows: Step 1: 94° C., 3 min; Step 2: 94° C., 15 sec; Step 3: 57° C., 1 min; Step 4: 68° C., 2 min; Step 5: Steps 2, 3, and 4 repeated 20 times; Step 6: 68° C., 5 min; Step 7: storage at 4° C.

[0130] The concentration of DNA in each well was determined by dispensing 100 μl PICOGREEN reagent (0.25% reagent in 1× TE, v/v; Molecular Probes) and 0.5 μl of undiluted PCR product into each well of an opaque fluorimeter plate (Corning Costar, Acton Mass.) and allowing the DNA to bind to the reagent. The plate was scanned in a FLUOROSKAN II (Labsystems Oy) to measure the fluorescence of the sample and to quantify the concentration of DNA. A 5 μl to 10 μl aliquot of the reaction mixture was analyzed by electrophoresis on a 1% agarose mini-gel to determine which reactions were successful in extending the sequence.

[0131] The extended nucleic acids were desalted and concentrated, transferred to 384-well plates, digested with CviJI cholera virus endonuclease (Molecular Biology Research, Madison Wis.), and sonicated or sheared prior to religation into pUC18 vector (APB). For shotgun sequencing, the digested nucleic acids were separated on low concentration (0.6 to 0.8%) agarose gels, fragments were excised, and agar digested with AGARACE enzyme (Prorega). Extended clones were religated using T4 DNA ligase (New England Biolabs, Beverly Mass.) into pUC18 vector (APB), treated with Pfu DNA polymerase (Stratagene) to fill-in restriction site overhangs, and transformed into competent E. coli cells. Transformed cells were selected on antibiotic-containing media, and individual colonies were picked and cultured overnight at 37° C. in 384-well plates in LB/2× carbenicillin liquid media.

[0132] The cells were lysed, and DNA was amplified by PCR using Taq DNA polymerase (APB) and Pfu DNA polymerase (Stratagene) with the following parameters: Step 1: 94° C., 3 min; Step 2: 94° C., 15 sec; Step 3: 60° C., 1 min; Step 4: 72° C., 2 min; Step 5: steps 2, 3, and 4 repeated 29 times; Step 6: 72° C., 5 min; Step 7: storage at 4° C. DNA was quantified using PICOGREEN reagent (Molecular Probes) as described above. Samples with low DNA recoveries were reamplified using the same conditions described above. Samples were diluted with 20% dimethylsulfoxide (DMSO; 1:2, v/v), and sequenced using DYENAMIC energy transfer sequencing primers and the DYENAMIC DIRECT cycle sequencing kit (APB) or the ABI PRISM BIGDYE terminator cycle sequencing kit (Applied Biosystems).

[0133] IV Assembly and Analysis of Sequences

[0134] Component nucleotide sequences from chromatograms were subjected to PHRED analysis (Phil Green, University of Washington, Seattle Wash.) and assigned a quality score. The sequences having at least a required quality score were subject to various pre-processing algorithms to eliminate low quality 3′ ends, vector and linker sequences, polyA tails, Alu repeats, mitrochondrial and ribosomal sequences, bacterial contamination sequences, and sequences smaller than 50 base pairs. Sequences were screened using the BLOCK 2 program (Incyte Genomics), a motif analysis program based on sequence information contained in the SWISS-PROT and PROSITE databases (Bairoch et al. (1997) Nucleic Acids Res 25:217-221; Attwood et al. (1997) J Chem Inf Comput Sci 37:417-424).

[0135] Processed sequences were subjected to assembly procedures in which the sequences were assigned to bins, one sequence per bin. Sequences in each bin were assembled to produce consensus sequences, templates. Subsequent new sequences were added to existing bins using BLAST (Altschul (supra); Altschul et al. (supra); Karlin et al. (1988) Proc Natl Acad Sci 85:841-845), BLASTn (vers.1.4, WashU), and CROSSMATCH software (Phil Green, supra). Candidate pairs were identified as all BLAST hits having a quality score greater than or equal to 150. Alignments of at least 82% local identity were accepted into the bin. The component sequences from each bin were assembled using PHRAP (Phil Green, supra). Bins with several overlapping component sequences were assembled using DEEP PHRAP (Phil Green, supra).

[0136] Bins were compared against each other, and those having local similarity of at least 82% were combined and reassembled. Reassembled bins having templates of insufficient overlap (less than 95% local identity) were re-split. Assembled templates were also subjected to analysis by STITCHER/EXON MAPPER algorithms which analyzed the probabilities of the presence of splice variants, alternatively spliced exons, splice junctions, differential expression of alternative spliced genes across tissue types, disease states, and the like. These resulting bins were subjected to several rounds of the above assembly procedures to generate the template sequences found in the LIFESEQ GOLD database (Incyte Genomics).

[0137] The assembled templates were annotated using the following procedure. Template sequences were analyzed using BLASTn (vers. 2.0, NCBI) versus GBpri (GenBank vers. 116). “Hits” were defined as an exact match having from 95% local identity over 200 base pairs through 100% local identity over 100 base pairs, or a homolog match having an E-value equal to or greater than 1×10⁻⁸. (The “E-value” quantifies the statistical probability that a match between two sequences occurred by chance). The hits were subjected to frameshift FASTx versus GENPEPT (GenBank version 109). In this analysis, a homolog match was defined as having an E-value of 1×10⁻⁸. The assembly method used above was described in U.S. Ser. No. 09/276,534, filed Mar. 25, 1999, and the LIFESEQ GOLD user manual (Incyte Genomics).

[0138] Following assembly, template sequences were subjected to motif, BLAST, Hidden Markov Model (HMM; Pearson and Lipman (1988) Proc Natl Acad Sci 85:2444-2448; Smith and Waterman (1981) J Mol Biol 147:195-197), and functional analyses, and categorized in protein hierarchies using methods described in U.S. Ser. No. 08/812,290, filed Mar. 6, 1997; U.S. Ser. No. 08/947,845, filed Oct. 9, 1997; U.S. Pat. No. 5,953,727; and U.S. Ser. No. 09/034,807, filed Mar. 4, 1998. Template sequences may be further queried against public databases such as the GenBank rodent, mammalian, vertebrate, eukaryote, prokaryote, and human EST databases.

[0139] V Selection of Sequences, Microarray Preparation and Use

[0140] Incyte clones represent template sequences derived from the LIFESEQ GOLD assembled human sequence database (Incyte Genomics). In cases where more than one clone was available for a particular template, the 5′-most clone in the template was used on the microarray. The HUMAN GENOME GEM series 1-3 microarrays (Incyte Pharmaceuticals) contain 28,626 array elements which represent 10,068 annotated clusters and 18,558 unannotated clusters. Tables 1 and 2 show the GenBank annotations for SEQ ID NOs:1-x of this invention as produced by BLAST analysis.

[0141] To construct microarrays, cDNAs were amplified from bacterial cells using primers complementary to vector sequences flanking the cDNA insert. Thirty cycles of PCR increased the initial quantity of cDNAs from 1-2 ng to a final quantity greater than 5 μg. Amplified cDNAs were then purified using SEPHACRYL-400 columns (APB). Purified cDNAs were immobilized on polymer-coated glass slides. Glass microscope slides (Corning, Corning N.Y.) were cleaned by ultrasound in 0.1% SDS and acetone, with extensive distilled water washes between and after treatments. Glass slides were etched in 4% hydrofluoric acid (VWR Scientific Products, West Chester Pa.), washed thoroughly in distilled water, and coated with 0.05% aminopropyl silane (Sigma Aldrich) in 95% ethanol. Coated slides were cured in a 110° C. oven. cDNAs were applied to the coated glass substrate using a procedure described in U.S. Pat. No. 5,807,522. One microliter of the cDNA at an average concentration of 100 ng/ul was loaded into the open capillary printing element by a high-speed robotic apparatus which then deposited about 5 nl of cDNA per slide.

[0142] Microarrays were UV-crosslinked using a STRATALINKER UV-crosslinker (Stratagene), and then washed at room temperature once in 0.2% SDS and three times in distilled water. Non-specific binding sites were blocked by incubation of microarrays in 0.2% casein in phosphate buffered saline (Tropix, Bedford Mass.) for 30 minutes at 60° C. followed by washes in 0.2% SDS and distilled water as before.

[0143] VI Preparation of Samples

[0144] The following cell lines were obtained from American Type Culture Collection (Manassus Va.) and cultured in media according to the manufacturer's protocols: PZ-HPV-7 was derived from epithelial cells cultured from normal tissue from the peripheral zone of the prostate. CA-HPV-10 was derived from cells from a prostatic adenocarcinoma of Gleason Grade 4/4. Both PZ cells were transformed by transfection with human papillomavirus (HPV)-18, and express keratins 5 and 8 and the early region 6 oncoprotein of HPV. PZ-HPV-7 and CA-HPV-10 are negative for prostate specific antigen (PSA). DU-145 is a prostate carcinoma cell line isolated from a 69 year-old man with widespread metastatic disease. DU-145 was isolated from a brain metastasis and has no detectable hormone sensitivity. Further, DU-145 is negative for PSA; PC-3 is a prostate adenocarcinoma cell line isolated from a 62 year-old male with grade IV prostate adenocarcinoma metastasized to the bone. PC-3 cells exhibit low acid phosphatase and testosterone-5-alpha reductase activities; LNCaP is a prostate carcinoma cell line isolated from a lymph node biopsy of a 50 year-old male with metastatic prostate carcinoma. LNCaP cells are responsive to 5-alpha-dihydrotestosterone and express androgen receptors.

[0145] PrEC, a primary prostate epithelial cell line isolated from a normal donor, was obtained from Clinomics Corporation (Walkersville Md.) and cultured in media according to the manufacturer's protocols.

[0146] All cultures were maintained at 37° C. and 5% CO₂ for 3-5 passages.

[0147] Isolation and Labeling of Sample cDNAs

[0148] Cells were harvested when cultures were approximately 70% confluent and lysed in 1 ml of TRIZOL reagent (5×10⁶ cells/ml; Life Technologies). The lysates were vortexed thoroughly and incubated at room temperature for 2-3 minutes and extracted with 0.5 ml chloroform. The extract was mixed, incubated at room temperature for 5 minutes, and centrifuged at 15,000 rpm for 15 minutes at 4° C. The aqueous layer was collected and an equal volume of isopropanol was added. Samples were mixed, incubated at room temperature for 10 minutes, and centrifuged at 15,000 rpm for 20 minutes at 4° C. The supernatant was removed and the RNA pellet was washed with 1 ml of 70% ethanol, centrifuged at 15,000 rpm at 4° C., and resuspended in RNase-free water. The concentration of the RNA was determined by measuring the optical density at 260 mm.

[0149] Poly(A) RNA was prepared using an OLIGOTEX mRNA kit (QIAGEN) with the following modifications: OLIGOTEX beads were washed in tubes instead of on spin columns, resuspended in elution buffer, and then loaded onto spin columns to recover mRNA. To obtain maximum yield, the mRNA was eluted twice.

[0150] Each poly(A) RNA sample was reverse transcribed using MMLV reverse-transcriptase, 0.05 pg/μl oligo-d(T) primer (21 mer), 1× first strand buffer, 0.03 units/ul RNase inhibitor, 500 uM dATP, 500 uM dGTP, 500 uM dTTP, 40 uM dCTP, and 40 uM either dCTP-Cy3 or dCTP-CyS (APB). The reverse transcription reaction was performed in a 25 ml volume containing 200 ng poly(A) RNA using the GEMBRIGHT kit (Incyte Pharmaceuticals). Specific control poly(A) RNAs (YCFR06, YCFR45, YCFR67, YCFR85, YCFR43, YCFR22, YCFR23, YCFR25, YCFR44, YCFR26) were synthesized by in vitro transcription from non-coding yeast genomic DNA (W. Lei, unpublished). As quantitative controls, control mRNAs (YCFR06, YCFR45, YCFR67, and YCFR85) at 0.002 ng, 0.02 ng, 0.2 ng, and 2 ng were diluted into reverse transcription reaction at ratios of 1:100,000, 1:10,000, 1:1000, 1:100 (w/w) to sample mRNA, respectively. To sample differential expression patterns, control mRNAs (YCFR43, YCFR22, YCFR23, YCFR25, YCFR44, YCFR26) were diluted into reverse transcription reaction at ratios of 1:3, 3:1, 1:10, 10:1, 1:25, 25:1 (w/w) to sample mRNA. Reactions were incubated at 37° C. for 2 hr, treated with 2.5 ml of 0.5M sodium hydroxide, and incubated for 20 minutes at 85° C. to the stop the reaction and degrade the RNA.

[0151] cDNAs were purified using two successive CHROMA SPIN 30 gel filtration spin columns (Clontech). Cy3- and CyS-labeled reaction samples were combined as follows: Aliquots of Cy3-labeled PrEC cDNA were individually mixed with CyS labeled cDNA from PZ-HPV-7, CA-HPV-10, DU-145, PC-3, and LNCaP cells. The mixtures were ethanol precipitated using 1 ml of glycogen (1 mg/ml), 60 rn sodium acetate, and 300 ml of 100% ethanol, dried to completion using a SpeedVAC system (Savant Instruments, Holbrook N.Y.), and resuspended in 14 μl 5×SSC/0.2% SDS.

[0152] VII Hybridization and Detection

[0153] Hybridization reactions contained 9 μl of sample mixture containing 0.2 μg each of Cy3 and CyS labeled cDNA synthesis products in 5×SSC, 0.2% SDS hybridization buffer. The mixture was heated to 65° C. for 5 minutes and was aliquoted onto the microarray surface and covered with an 1.8 cm² coverslip. The microarrays were transferred to a waterproof chamber having a cavity just slightly larger than a microscope slide. The chamber was kept at 100% humidity internally by the addition of 140 μl of 5× SSC in a corner of the chamber. The chamber containing the microarrays was incubated for about 6.5 hours at 60° C. The microarrays were washed for 10 min at 45° C. in low stringency wash buffer (1×SSC, 0.1% SDS), three times for 10 minutes each at 45° C. in high stringency wash buffer (0.1×SSC), and dried.

[0154] Reporter-labeled hybridization complexes were detected with a microscope equipped with an Innova 70 mixed gas 10 W laser (Coherent, Santa Clara Calif.) capable of generating spectral lines at 488 nm for excitation of Cy3 and at 632 nm for excitation of Cy5. The excitation laser light was focused on the microarray using a 20×microscope objective (Nikon, Melville N.Y.). The slide containing the microarray was placed on a computer-controlled X-Y stage on the microscope and raster-scanned past the objective. The 1.8 cm×1.8 cm microarray used in the present example was scanned with a resolution of 20 micrometers.

[0155] In two separate scans, the mixed gas multiline laser excited the two fluorophores sequentially. Emitted light was split, based on wavelength, into two photomultiplier tube detectors (PMT R1477; Hamamatsu Photonics Systems, Bridgewater N.J.) corresponding to the two fluorophores. Appropriate filters positioned between the microarray and the photomultiplier tubes were used to filter the signals. The emission maxima of the fluorophores used were 565 nm for Cy3 and 650 nm for CyS. Each microarray was typically scanned twice, one scan per fluorophore using the appropriate filters at the laser source, although the apparatus was capable of recording the spectra from both fluorophores simultaneously.

[0156] The sensitivity of the scans was calibrated using the signal intensity generated by a cDNA control species. Samples of the calibrating cDNA were separately labeled with the two fluorophores and identical amounts of each were added to the hybridization mixture. A specific location on the microarray contained a complementary DNA sequence, allowing the intensity of the signal at that location to be correlated with a weight ratio of hybridizing species of 1:100,000.

[0157] The output of the photomultiplier tube was digitized using a 12-bit RTI-835H analog-to-digital (A/D) conversion board (Analog Devices, Norwood, Mass.) installed in an IBM-compatible PC computer. The digitized data were displayed as an image where the signal intensity was mapped using a linear 20-color transformation to a pseudocolor scale ranging from blue (low signal) to red (high signal). The data was also analyzed quantitatively. Where two different fluorophores were excited and measured simultaneously, the data were first corrected for optical crosstalk (due to overlapping emission spectra) between the fluorophores using each fluorophore's emission spectrum

[0158] A grid was superimposed over the fluorescence signal image such that the signal from each spot was centered in each element of the grid. The fluorescence signal within each element was then integrated to obtain a numerical value corresponding to the average intensity of the signal. The software used for signal analysis was the GEMTOOLS gene expression analysis program (Incyte Pharmaceuticals). Significance was defined as signal to background ratio exceeding 2× and area hybridization exceeding 40%.

[0159] VIII Data Analysis and Results

[0160] Array elements that exhibited at least 2.5-fold change in expression at one or more time points, a signal intensity over 250 units, a signal-to-background ratio of at least 2.5, and an element spot size of at least 40% were identified as differentially expressed using the GEMTOOLS program (Incyte Genomics). Differential expression values were converted to log base 2 scale. Differential expression values were then compared between the cell lines to identify genes which discriminated between normal and cancerous and between non-metastatic and metastatic cancer. The student's t-test and Pearson correlation statistics were used to distinguish significant differences between the groups. The resulting cDNAs are shown in Tables 1 and 2. The cDNAs are identified by their Clone ID. Table 3 shows the sequence overlap between the clones identified in Tables 1 and 2 and gene templates. Columns 1-3 show the SEQ ID NO:, Template ID, and Clone ID, respectively. Columms 4 and 5 show the start and stop nucleotides for the clone on the template. Table 4 shows a GenBank homolog and description associated with at least a fragment of each Template ID. The descriptions were obtained using the sequences of the Sequence Listing and BLAST analysis. SEQ ID NOs:1-3, 5, 6, 8, 10-15, 17-19, 21, 23-28, 30, 32, 34-36, 38, 40, 42-45, 47-50, 52, 53, 55, 56, 58-65, 67, 68, 70-73, 75 are highly correlated with metastatic prostate cancer cells PC-3, LNCaP, and DU-145, and SEQ ID NOs:76, 78-86, 88-90, 92-97, 99-101 are differentially expressed at significant levels in all of the prostate cancer cell lines.

[0161] IX Other Hybridization Technologies and Analyses

[0162] Other hybridization technologies utilize a variety of substrates such as nylon membranes, capillary tubes, etc. Arranging cDNAs on polymer coated slides is described in Example V; sample cDNA preparation and hybridization and analysis using polymer coated slides is described in examples VI and VII, respectively. cDNAs are applied to a membrane substrate by one of the following methods. A mixture of cDNAs is fractionated by gel electrophoresis and transferred to a nylon membrane by capillary transfer. Alternatively, the cDNAs are individually ligated to a vector and inserted into bacterial host cells to form a library. The cDNAs are then arranged on a substrate by one of the following methods. In the first method, bacterial cells containing individual clones are robotically picked and arranged on a nylon membrane. The membrane is placed on LB agar containing selective agent (carbenicillin, kanamycin, ampicillin, or chloramphenicol depending on the vector used) and incubated at 37° C. for 16 hr. The membrane is removed from the agar and consecutively placed colony side up in 10% SDS, denaturing solution (1.5 M NaCl, 0.5 M NaOH), neutralizing solution (1.5 M NaCl, 1 M Tris, pH 8.0), and twice in 2×SSC for 10 min each. The membrane is then UV irradiated in a STRATALINKER UV-crosslinker (Stratagene).

[0163] In the second method, cDNAs are amplified from bacterial vectors by thirty cycles of PCR using primers complementary to vector sequences flanking the insert. PCR amplification increases a starting concentration of 1-2 ng nucleic acid to a final quantity greater than 5 μg. Amplified nucleic acids from about 400 bp to about 5000 bp in length are purified using SEPHACRYL-400 beads (APB). Purified nucleic acids are arranged on a nylon membrane manually or using a dot/slot blotting manifold and suction device and are immobilized by denaturation, neutralization, and UV irradiation as described above.

[0164] Hybridization probes derived from cDNAs of the Sequence Listing are employed for screening cDNAs, mRNAs, or genomic DNA in membrane-based hybridizations. Probes are prepared by diluting the cDNAs to a concentration of 40-50 ng in 45 μl TE buffer, denaturing by heating to 100° C. for five min and briefly centrifuging. The denatured cDNA is then added to a REDIPRIME tube (APB), gently mixed until blue color is evenly distributed, and briefly centrifuged. Five microliters of [³²P]dCTP is added to the tube, and the contents are incubated at 37° C. for 10 min. The labeling reaction is stopped by adding 5 μl of 0.2M EDTA, and probe is purified from unincorporated nucleotides using a PROBEQUANT G-50 microcolumn (APB). The purified probe is heated to 100° C. for five min and then snap cooled for two min on ice.

[0165] Membranes are pre-hybridized in hybridization solution containing 1% Sarkosyl and 1×high phosphate buffer (0.5 M NaCl, 0.1 M Na₂HPO₄, 5 mM EDTA, pH 7) at 55° C. for two hr. The probe, diluted in 15 ml fresh hybridization solution, is then added to the membrane. The membrane is hybridized with the probe at 55° C. for 16 hr. Following hybridization, the membrane is washed for 15 min at 25° C. in 1 mM Tris (pH 8.0), 1% Sarkosyl, and four times for 15 min each at 25° C. in 1 mM Tris (pH 8.0). To detect hybridization complexes, XOMAT-AR filn (Eastman Kodak, Rochester N.Y.) is exposed to the membrane overnight at −70° C., developed, and examined.

[0166] X Further Characterization of Differentially Expressed cDNAs and Proteins

[0167] Clones were blasted against the LIFESEQ Gold 5.1 database (Incyte Genomics) and an Incyte template and its sequence variants were chosen for each clone. The template and variant sequences were blasted against GenBank database to acquire annotation. The nucleotide sequences were translated into amino acid sequence which was blasted against the GenPept and other protein databases to acquire annotation and characterization, i.e., structural motifs.

[0168] Percent sequence identity can be determined electronically for two or more amino acid or nucleic acid sequences using the MEGALIGN program (DNASTAR). The percent identity between two amino acid sequences is calculated by dividing the length of sequence A, minus the number of gap residues in sequence A, minus the number of gap residues in sequence B, into the sum of the residue matches between sequence A and sequence B, times one hundred. Gaps of low or of no homology between the two amino acid sequences are not included in determining percentage identity.

[0169] Sequences with conserved protein motifs may be searched using the BLOCKS search program. This program analyses sequence information contained in the Swiss-Prot and PROSITE databases and is useful for determining the classification of uncharacterized proteins translated from genomic or cDNA sequences (Bairoch et al. (supra); Attwood et al. (supra). PROSITE database is a useful source for identifying functional or structural domains that are not detected using motifs due to extreme sequence divergence. Using weight matrices, these domains are calibrated against the SWISS-PROT database to obtain a measure of the chance distribution of the matches.

[0170] The PRINTS database can be searched using the BLIMPS search program to obtain protein family “fingerprints”. The PRINTS database complements the PROSITE database by exploiting groups of conserved motifs within sequence alignments to build characteristic signatures of different protein families. For both BLOCKS and PRINTS analyses, the cutoff scores for local similarity were: >1300=strong, 1000-1300=suggestive; for global similarity were: p<exp-3; and for strength (degree of correlation) were: >1300=strong, 1000-1300=weak.

[0171] X Expression of the Encoded Protein

[0172] Expression and purification of a protein encoded by a cDNA of the invention is achieved using bacterial or virus-based expression systems. For expression in bacteria, cDNA is subcloned into a vector containing an antibiotic resistance gene and an inducible promoter that directs high levels of cDNA transcription. Examples of such promoters include, but are not limited to, the trp-lac (tac) hybrid promoter and the T5 or T7 bacteriophage promoter in conjunction with the lac operator regulatory element. Recombinant vectors are transformed into bacterial hosts, such as BL21 (DE3). Antibiotic resistant bacteria express the protein upon induction with IPTG. Expression in eukaryotic cells is achieved by infecting Spodoptera frugiperda (Sf9) insect cells with recombinant baculovirus, Autographica californica nuclear polyhedrosis virus. The polyhedrin gene of baculovirus is replaced with the cDNA by either homologous recombination or bacterial-mediated transposition involving transfer plasmid intermediates. Viral infectivity is maintained and the strong polyhedrin promoter drives high levels of transcription.

[0173] For ease of purification, the protein is synthesized as a fusion protein with glutathione-S-transferase (GST; APB) or a similar alternative such as FLAG. The fusion protein is purified on immobilized glutathione under conditions that maintain protein activity and antigenicity. After purification, the GST moiety is proteolytically cleaved from the protein with thrombin. A fusion protein with FLAG, an 8-amino acid peptide, is purified using commercially available monoclonal and polyclonal anti-FLAG antibodies (Eastman Kodak, Rochester N.Y.).

[0174] XI Production of Specific Antibodies

[0175] A denatured protein from a reverse phase HPLC separation is obtained in quantities up to 75 mg. This denatured protein is used to immunize mice or rabbits following standard protocols. About 100 μg is used to immunize a mouse, while up to 1 mg is used to immunize a rabbit. The denatured protein is radioiodinated and incubated with murine B-cell hybridomas to screen for monoclonal antibodies. About 20 mg of protein is sufficient for labeling and screening several thousand clones.

[0176] In another approach, the amino acid sequence translated from a cDNA of the invention is analyzed using PROTEAN software (DNASTAR) to determine regions of high antigenicity, essentially antigenically-effective epitopes of the protein. The optimal sequences for immunization are usually at the C-terminus, the N-terminus, and those intervening, hydrophilic regions of the protein that are likely to be exposed to the external environment when the protein is in its natural conformation. Typically, oligopeptides about 15 residues in length are synthesized using an ABI 431 peptide synthesizer (Applied Biosystems) using Fmoc-chemistry and then coupled to keyhole limpet hemocyanin (KLH; Sigma Aldrich) by reaction with M-maleimidobenzoyl-N-hydroxysuccinimide ester. If necessary, a cysteine may be introduced at the N-terminus of the peptide to permit coupling to KLH. Rabbits are immunized with the oligopeptide-KLH complex in complete Freund's adjuvant. The resulting antisera are tested for antipeptide activity by binding the peptide to plastic, blocking with 1% BSA, reacting with rabbit antisera, washing, and reacting with radioiodinated goat anti-rabbit IgG.

[0177] Hybridomas are prepared and screened using standard techniques. Hybridomas of interest are detected by screening with radioiodinated protein to identify those fusions producing a monoclonal antibody specific for the protein. In a typical protocol, wells of 96 well plates (FAST, Becton-Dickinson, Palo Alto Calif.) are coated with affinity-purified, specific rabbit-anti-mouse (or suitable anti-species Ig) antibodies at 10 mg/ml. The coated wells are blocked with 1% BSA and washed and exposed to supernatants from hybridomas. After incubation, the wells are exposed to radiolabeled protein at 1 mg/ml. Clones producing antibodies bind a quantity of labeled protein that is detectable above background.

[0178] Such clones are expanded and subjected to 2 cycles of cloning at 1 cell/3 wells. Cloned hybridomas are injected into pristane-treated mice to produce ascites, and monoclonal antibody is purified from the ascitic fluid by affinity chromatography on protein A (APB). Monoclonal antibodies with affinities of at least 10⁸ M⁻¹, preferably 10⁹ to 10¹⁰ M⁻¹ or stronger, are made by procedures well known in the art.

[0179] XII Purification of Naturally Occurring Protein Using Specific Antibodies

[0180] Naturally occurring or recombinant protein is substantially purified by immunoaffinity chromatography using antibodies specific for the protein. An immunoaffinity column is constructed by covalently coupling the antibody to CNBr-activated SEPHAROSE resin (APB). Media containing the protein is passed over the immunoaffinity column, and the column is washed using high ionic strength buffers in the presence of detergent to allow preferential absorbance of the protein. After coupling, the protein is eluted from the column using a buffer of pH 2-3 or a high concentration of urea or thiocyanate ion to disrupt antibody/protein binding, and the protein is collected.

[0181] XIII Screening Molecules for Specific Binding with the cDNA or Protein

[0182] The cDNA or fragments thereof and the protein or portions thereof are labeled with ³²P-dCTP, Cy3-dCTP, Cy5-dCTP (APB), or BIODIPY or FITC (Molecular Probes), respectively. Candidate molecules or compounds previously arranged on a substrate are incubated in the presence of labeled nucleic or amino acid. After incubation under conditions for either a cDNA or a protein, the substrate is washed, and any position on the substrate retaining label, which indicates specific binding or complex formation, is assayed. The binding molecule is identified by its arrayed position on the substrate. Data obtained using different concentrations of the nucleic acid or protein are used to calculate affinity between the labeled nucleic acid or protein and the bound molecule. High throughput screening using very small assay volumes and very small amounts of test compound is fully described in Burbaum et al. U.S. Pat. No. 5,876,946.

[0183] All patents and publications mentioned in the specification are incorporated herein by reference. Various modifications and variations of the described method and system of the invention will be apparent to those skilled in the art without departing from the scope and spirit of the invention. Although the invention has been described in connection with specific preferred embodiments, it should be understood that the invention as claimed should not be unduly limited to such specific embodiments. Indeed, various modifications of the described modes for carrying out the invention that are obvious to those skilled in the field of molecular biology or related fields are intended to be within the scope of the following claims.

1 102 1 1645 DNA Homo sapiens misc_feature Incyte ID No 1382961.3 1 cctttccaat ttacccgagc accttctctt cactcagcca actgctcgct cgctcacctc 60 cctcctctgc accatgacta cctgcagccg ccagttcacc tcctccagct ccatgaaggg 120 ctcctgcggc atcgggggcg gcatcggggg cggctccagc cgcatctcct ccgtcctggc 180 cggagggtcc tgccgcgccc ccagcaccta cgggggcggc ctgtctgtct catcctcccg 240 cttctcctct gggggagcct atgggttggg gggcggctat ggcggtggct tcagcagcag 300 aaccagcagc tttggtagtg gctttggggg aggatatggt ggtggccttg gtgctggctt 360 gggtggtggc tttggtggtg gctttgctgg tggtgatggg cttctggtgg gcagtgagaa 420 ggtgaccatg cagaacctca acgaccgcct ggcctcctac ctggacaagg tgcgtgctct 480 ggaggaggcc aacgccgacc tggaagtgaa gatccgtgac tggtaccaga ggcagcggcc 540 tgctgagatc aaagactaca gtccctactt caagaccatt gaggacctga ggaacaagat 600 tctcacagcc acagtggaca atgccaatgt ccttctgcag attgacaatg cccgtctggc 660 cgcggatgac ttccgcacca agtatgagac agagttgaac ctgcgcatga gtgtggaagc 720 cgacatcaat ggcctgcgca gggtgctgga cgaactgacc ctggccagag ctgacctgga 780 gatgcagatt gagagcctga aggaggagct ggcctacctg aagaagaacc acgaggagga 840 gatgaatgcc ctgagaggcc aggtgggtgg agatgtcaat gtggagatgg acgctgcacc 900 tggcgtggac ctgagccgca ttctgaacga gatgcgtgac cagtatgaga agatggcaga 960 gaagaaccgc aaggatgccg aggaatggtt cttcaccaag acagaggagc tgaaccgcga 1020 ggtggccacc aacagcgagc tggtgcagag cggcaagagc gagatctcgg agctccggcg 1080 caccatgcag aacctggaga ttgagctgca gtcccagctc agcatgaaag catccctgga 1140 gaacagcctg gaggagacca aaggtcgcta ctgcatgcag ctggcccaga tccaggagat 1200 gattggcagc gtggaggagc agctggccca gctccgctgc gagatggagc agcagaacca 1260 ggagtacaag atcctgctgg acgtgaagac gcggctggag caggagatcg ccacctaccg 1320 ccgcctgctg gagggcgagg acgcccacct ctcctcctcc cagttctcct ctggatcgca 1380 gtcatccaga gatgtgacct cctccagccg ccaaatccgc accaaggtca tggatgtgca 1440 cgatggcaag gtggtgtcca cccacgagca ggtccttcgc accaagaact gaggctgccc 1500 agccccgctc aggcctagga ggccccccgt gtggacacag atcccactgg aagatcccct 1560 ctcctgccca agcacttcac agctggaccc tgcttcaccc tcaccccctc ctggcaatca 1620 atacagcttc attatctgag ttgca 1645 2 1051 DNA Homo sapiens misc_feature Incyte ID No 1382961.5 2 agcaaatgcc ttctccctgc atgctccctg caaggcctcc tcgctatctc cacacacctg 60 actcatccca ttttacagga gcagttgatc ccaggaagag cattggagcc tccagcaggg 120 gctgttgggg cctgtctgag gagataggat gcgtcaggca gccccagaca cgatcacatt 180 cctctcaaca tgcctgccgg gccgggtatc catcccctgc agcagcaggc ttcctctacg 240 tggatgttaa aggcccattc agttcatgga gagctagcag gtgcgtgctc tggaggaggc 300 caacgccgac ctggaagtga agatccgtga ctggtaccag aggcagcggc ctgctgagat 360 caaagactac agtccctact tcaagaccat tgaggacctg aggaacaaga ttctcacagc 420 cacagtggac aatgccaatg tccttctgca gattgacaat gcccgtctgg ccgcggatga 480 cttccgcacc aagtatgaga cagagttgaa cctgcgcatg agtgtggaag ccgaccatca 540 atggcctgcg cagggtgctg gacgaactga cctggccaga gctgacctgg agatgcagat 600 tgagagcctg aaggaggagc tggcctacct gaagaagaac cacgaggagg agatgaatgc 660 cctgagaggc caggtgggtg gagatgtcaa tgtggagatg gacgctgcac ctggcgtgga 720 cctgagccgc attctgaacg agatgcgtga ccagtatgag aagatggcag agaagaaccg 780 caaggatgcc gaggaatggt tcttcaccaa gacagaggag ctgaaccgcg aggtggccac 840 caacagcgag ctggtgcaga gcggcaagag cgagatctcg gagctccggc gcaccatgca 900 gaacctggag atgattggca gcgtggagga gcagctggcc cagctccgct gcgagatgga 960 gcagcagaac caggagtaca agatcctgct ggacgtgaag acgcggctgg agcaggagat 1020 cgccacctac cgccgcctgc tggagggcga g 1051 3 1930 DNA Homo sapiens misc_feature Incyte ID No 2852561CB1 3 ccttaagggg cgggccgggg cggggctccg ctgccccttc ccagaggccg cgcctgctgc 60 tgagcagatg cagtagccga aactgcgcgg aggcacagag gccggggaga gcgttctggg 120 tccgagggtc caggtagggg ttgagccacc atctgaccgc aagctgcgtc gtgtcgccgg 180 ttctgcaggc accatgagcc aggacaccga ggtggatatg aaggaggtgg agctgaatga 240 gttagagccc gagaagcagc cgatgaacgc ggcgtctggg gcggccatgt ccctggcggg 300 agccgagaag aatggtctgg tgaagatcaa ggtggcggaa gacgaggcgg aggcggcagc 360 cgcggctaag ttcacgggcc tgtccaagga ggagctgctg aaggtggcag gcagccccgg 420 ctgggtacgc acccgctggg cactgctgct gctcttctgg ctcggctggc tcggcatgct 480 tgctggtgcc gtggtcataa tcgtgcgagc gccgcgttgt cgcgagctac cggcgcagaa 540 gtggtggcac acgggcgccc tctaccgcat cggcgacctt caggccttcc agggccacgg 600 cgcgggcaac ctggcgggtc tgaaggggcg tctcgattac ctgagctctc tgaaggtgaa 660 gggccttgtg ctgggtccaa ttcacaagaa ccagaaggat gatgtcgctc agactgactt 720 gctgcagatc gaccccaatt ttggctccaa ggaagatttt gacagtctct tgcaatcggc 780 taaaaaaaag agcatccgtg tcattctgga ccttactccc aactaccggg gtgagaactc 840 gtggttctcc actcaggttg acactgtggc caccaaggtg aaggatgctc tggagttttg 900 gctgcaagct ggcgtggatg ggttccaggt tcgggacata gagaatctga aggatgcatc 960 ctcattcttg gctgagtggc aaaatatcac caagggcttc agtgaagaca ggctcttgat 1020 tgcggggact aactcctccg accttcagca gatcctgagc ctactcgaat ccaacaaaga 1080 cttgctgttg actagctcat acctgtctga ttctggttct actggggagc atacaaaatc 1140 cctagtcaca cagtatttga atgccactgg caatcgctgg tgcagctgga gtttgtctca 1200 ggcaaggctc ctgacttcct tcttgccggc tcaacttctc cgactctacc agctgatgct 1260 cttcaccctg ccagggaccc ctgttttcag ctacggggat gagattggcc tggatgcagc 1320 tgcccttcct ggacagccta tggaggctcc agtcatgctg tgggatgagt ccagcttccc 1380 tgacatccca ggggctgtaa gtgccaacat gactgtgaag ggccagagtg aagaccctgg 1440 ctccctcctt tccttgttcc ggcggctgag tgaccagcgg agtaaggagc gctccctact 1500 gcatggggac ttccacgcgt tctccgctgg gcctggactc ttctcctata tccgccactg 1560 ggaccagaat gagcgttttc tggtagtgct taactttggg gatgtgggcc tctcggctgg 1620 actgcaggcc tccgacctgc ctgccagcgc cagcctgcca gccaaggctg acctcctgct 1680 cagcacccag ccaggccgtg aggagggctc ccctcttgag ctggaacgcc tgaaactgga 1740 gcctcacgaa gggctgctgc tccgcttccc ctacgcggcc tgacttcagc ctgacatgga 1800 cccactaccc ttctcctttc cttcccaggc cctttggctt ctgatttttc tcttttttaa 1860 aaacaaacaa acaaactgtt gcagattatg agtgaacccc caaataggtg tttctgcctt 1920 caaataagaa 1930 4 529 PRT Homo sapiens misc_feature Incyte ID No 2852561CD1 4 Met Ser Gln Asp Thr Glu Val Asp Met Lys Glu Val Glu Leu Asn 1 5 10 15 Glu Leu Glu Pro Glu Lys Gln Pro Met Asn Ala Ala Ser Gly Ala 20 25 30 Ala Met Ser Leu Ala Gly Ala Glu Lys Asn Gly Leu Val Lys Ile 35 40 45 Lys Val Ala Glu Asp Glu Ala Glu Ala Ala Ala Ala Ala Lys Phe 50 55 60 Thr Gly Leu Ser Lys Glu Glu Leu Leu Lys Val Ala Gly Ser Pro 65 70 75 Gly Trp Val Arg Thr Arg Trp Ala Leu Leu Leu Leu Phe Trp Leu 80 85 90 Gly Trp Leu Gly Met Leu Ala Gly Ala Val Val Ile Ile Val Arg 95 100 105 Ala Pro Arg Cys Arg Glu Leu Pro Ala Gln Lys Trp Trp His Thr 110 115 120 Gly Ala Leu Tyr Arg Ile Gly Asp Leu Gln Ala Phe Gln Gly His 125 130 135 Gly Ala Gly Asn Leu Ala Gly Leu Lys Gly Arg Leu Asp Tyr Leu 140 145 150 Ser Ser Leu Lys Val Lys Gly Leu Val Leu Gly Pro Ile His Lys 155 160 165 Asn Gln Lys Asp Asp Val Ala Gln Thr Asp Leu Leu Gln Ile Asp 170 175 180 Pro Asn Phe Gly Ser Lys Glu Asp Phe Asp Ser Leu Leu Gln Ser 185 190 195 Ala Lys Lys Lys Ser Ile Arg Val Ile Leu Asp Leu Thr Pro Asn 200 205 210 Tyr Arg Gly Glu Asn Ser Trp Phe Ser Thr Gln Val Asp Thr Val 215 220 225 Ala Thr Lys Val Lys Asp Ala Leu Glu Phe Trp Leu Gln Ala Gly 230 235 240 Val Asp Gly Phe Gln Val Arg Asp Ile Glu Asn Leu Lys Asp Ala 245 250 255 Ser Ser Phe Leu Ala Glu Trp Gln Asn Ile Thr Lys Gly Phe Ser 260 265 270 Glu Asp Arg Leu Leu Ile Ala Gly Thr Asn Ser Ser Asp Leu Gln 275 280 285 Gln Ile Leu Ser Leu Leu Glu Ser Asn Lys Asp Leu Leu Leu Thr 290 295 300 Ser Ser Tyr Leu Ser Asp Ser Gly Ser Thr Gly Glu His Thr Lys 305 310 315 Ser Leu Val Thr Gln Tyr Leu Asn Ala Thr Gly Asn Arg Trp Cys 320 325 330 Ser Trp Ser Leu Ser Gln Ala Arg Leu Leu Thr Ser Phe Leu Pro 335 340 345 Ala Gln Leu Leu Arg Leu Tyr Gln Leu Met Leu Phe Thr Leu Pro 350 355 360 Gly Thr Pro Val Phe Ser Tyr Gly Asp Glu Ile Gly Leu Asp Ala 365 370 375 Ala Ala Leu Pro Gly Gln Pro Met Glu Ala Pro Val Met Leu Trp 380 385 390 Asp Glu Ser Ser Phe Pro Asp Ile Pro Gly Ala Val Ser Ala Asn 395 400 405 Met Thr Val Lys Gly Gln Ser Glu Asp Pro Gly Ser Leu Leu Ser 410 415 420 Leu Phe Arg Arg Leu Ser Asp Gln Arg Ser Lys Glu Arg Ser Leu 425 430 435 Leu His Gly Asp Phe His Ala Phe Ser Ala Gly Pro Gly Leu Phe 440 445 450 Ser Tyr Ile Arg His Trp Asp Gln Asn Glu Arg Phe Leu Val Val 455 460 465 Leu Asn Phe Gly Asp Val Gly Leu Ser Ala Gly Leu Gln Ala Ser 470 475 480 Asp Leu Pro Ala Ser Ala Ser Leu Pro Ala Lys Ala Asp Leu Leu 485 490 495 Leu Ser Thr Gln Pro Gly Arg Glu Glu Gly Ser Pro Leu Glu Leu 500 505 510 Glu Arg Leu Lys Leu Glu Pro His Glu Gly Leu Leu Leu Arg Phe 515 520 525 Pro Tyr Ala Ala 5 664 DNA Homo sapiens misc_feature Incyte ID No 335942.2 5 ccaaaatgga gggaataata cctaagcctt cctgccgcaa cagtttttta tgctaatcag 60 ggaggtcatt ttggtaaaat acttcttgaa gccgagcctc aagatgaagg caaagcacga 120 aatgttattt tttaattatt atttatatat gtatttataa atatatttaa gataattata 180 atatactata tttatgggaa ccccttcatc ctctgagtgt gaccaggcat cctccacaat 240 agcagacagt gttttctggg ataagtaagt ttgatttcat taatacaggg cattttggtc 300 caagttgtgc ttatcccata gccaggaaac tctgcattct agtacttggg agacctgtaa 360 tcatataata aatgtacatt aattaccttg agccagtaat tggtccgatc tttgactctt 420 ttgccattaa acttacctgg gcattcttgt ttcaattcca cctgcaatca agtcctacaa 480 gctaaaatta gatgaactca actttgacaa ccatgagacc actgttatca aaactttctt 540 ttctggaatg taatcaatgt ttcttctagg ttctaaaaat tgtgatcaga ccataatgtt 600 acattattat caacaatagt gattgataga gtgttatcag tcataactaa ataaagcttg 660 caac 664 6 1667 DNA Homo sapiens misc_feature Incyte ID No 2483854CB1 6 gtcatttcat tggcgtttga gtcagcaaag aagtcaagat ggccaaagtt ccagacatgt 60 ttgaagacct gaagaactgt tacagtgaaa atgaagaaga cagttcctcc attgatcatc 120 tgtctctgaa tcagaaatcc ttctatcatg taagctatgg cccactccat gaaggctgca 180 tggatcaatc tgtgtctctg agtatctctg aaacctctaa aacatccaag cttaccttca 240 aggagagcat ggtggtagta gcaaccaacg ggaaggttct gaagaagaga cggttgagtt 300 taagccaatc catcactgat gatgacctgg aggccatcgc caatgactca gaggaagaaa 360 tcatcaagcc taggtcagca ccttttagct tcctgagcaa tgtgaaatac aactttatga 420 ggatcatcaa atacgaattc atcctgaatg acgccctcaa tcaaagtata attcgagcca 480 atgatcagta cctcacggct gctgcattac ataatctgga tgaagcagtg aaatttgaca 540 tgggtgctta taagtcatca aaggatgatg ctaaaattac cgtgattcta agaatctcaa 600 aaactcaatt gtatgtgact gcccaagatg aagaccaacc agtgctgctg aaggagatgc 660 ctgagatacc caaaaccatc acaggtagtg agaccaacct cctcttcttc tgggaaactc 720 acggcactaa gaactatttc acatcagttg cccatccaaa cttgtttatt gccacaaagc 780 aagactactg ggtgtgcttg gcaggggggc caccctctat cactgacttt cagatactgg 840 aaaaccaggc gtaggtctgg agtctcactt gtctcacttg tgcagtgttg acagttcata 900 tgtaccatgt acatgaagaa gctaaatcct ttactgttag tcatttgctg agcatgtact 960 gagccttgta attctaaatg aatgtttaca ctctttgtaa gagtggaacc aacactaaca 1020 tataatgttg ttatttaaag aacaccctat attttgcata gtaccaatca ttttaattat 1080 tattcttcat aacaatttta ggaggaccag agctactgac tatggctacc aaaaagactc 1140 tacccatatt acagatgggc aaattaaggc ataagaaaac taagaaatat gcacaatagc 1200 agttgaaaca agaagccaca gacctaggat ttcatgattt catttcaact gtttgccttc 1260 tacttttaag ttgctgatga actcttaatc aaatagcata agtttctggg acctcagttt 1320 tatcattttc aaaatggagg gaataatacc taagccttcc tgccgcaaca gttttttatg 1380 ctaatcaggg agggcatttt ggtaaaatac ttcttgaagc cgagcctcaa gatgaaggca 1440 aagcacgaaa tgttattttt taattattat ttatatatgt atttataaat atatttcaga 1500 taattataat atacctatat tgatgggaac ccttcatcct ctgaggtgtg accagggcat 1560 cctccacaat tagccgacag tggtttcctg gggataggta aggtttggtt tccattaata 1620 ccagggcatt ttgggtccaa gttgtgctta atcccataag ccaggga 1667 7 271 PRT Homo sapiens misc_feature Incyte ID No 2483854CD1 7 Met Ala Lys Val Pro Asp Met Phe Glu Asp Leu Lys Asn Cys Tyr 1 5 10 15 Ser Glu Asn Glu Glu Asp Ser Ser Ser Ile Asp His Leu Ser Leu 20 25 30 Asn Gln Lys Ser Phe Tyr His Val Ser Tyr Gly Pro Leu His Glu 35 40 45 Gly Cys Met Asp Gln Ser Val Ser Leu Ser Ile Ser Glu Thr Ser 50 55 60 Lys Thr Ser Lys Leu Thr Phe Lys Glu Ser Met Val Val Val Ala 65 70 75 Thr Asn Gly Lys Val Leu Lys Lys Arg Arg Leu Ser Leu Ser Gln 80 85 90 Ser Ile Thr Asp Asp Asp Leu Glu Ala Ile Ala Asn Asp Ser Glu 95 100 105 Glu Glu Ile Ile Lys Pro Arg Ser Ala Pro Phe Ser Phe Leu Ser 110 115 120 Asn Val Lys Tyr Asn Phe Met Arg Ile Ile Lys Tyr Glu Phe Ile 125 130 135 Leu Asn Asp Ala Leu Asn Gln Ser Ile Ile Arg Ala Asn Asp Gln 140 145 150 Tyr Leu Thr Ala Ala Ala Leu His Asn Leu Asp Glu Ala Val Lys 155 160 165 Phe Asp Met Gly Ala Tyr Lys Ser Ser Lys Asp Asp Ala Lys Ile 170 175 180 Thr Val Ile Leu Arg Ile Ser Lys Thr Gln Leu Tyr Val Thr Ala 185 190 195 Gln Asp Glu Asp Gln Pro Val Leu Leu Lys Glu Met Pro Glu Ile 200 205 210 Pro Lys Thr Ile Thr Gly Ser Glu Thr Asn Leu Leu Phe Phe Trp 215 220 225 Glu Thr His Gly Thr Lys Asn Tyr Phe Thr Ser Val Ala His Pro 230 235 240 Asn Leu Phe Ile Ala Thr Lys Gln Asp Tyr Trp Val Cys Leu Ala 245 250 255 Gly Gly Pro Pro Ser Ile Thr Asp Phe Gln Ile Leu Glu Asn Gln 260 265 270 Ala 8 1511 DNA Homo sapiens misc_feature Incyte ID No 1454852CB1 8 cccctctcct ccccagccct tctcctgtgt gcctgcctcc tgctgccctc accatgacca 60 cctccatccg ccagttcacc tcctccagct ccatcaaggg ctcctccggc ctggggggcg 120 gctcgtcccg cacctcctgc cggctgtctg gcggcctggg tgccggctcc tgcaggctgg 180 gatctgctgg cggcctgggc agcaccctcg ggggtagcag ctactccagc tgctacagct 240 ttggctctgg tggtggctat ggcagcagct ttgggggtgt tgatgggctg ctggctggag 300 gtgagaaggc caccatgcag aacctcaatg accgcctggc ctcctacctg gacaaggtgc 360 gtgccctgga ggaggccaac actgagctgg aggtgaagat ccgtgactgg taccagaggc 420 aggccccggg gcccgcccgt gactacagcc agtactacag gacaattgag gagctgcaga 480 acaagatcct cacagccacc gtggacaatg ccaacatcct gctacagatt gacaatgccc 540 gtctggctgc tgatgacttc cgcaccaagt ttgagacaga gcaggccctg cgcctgagtg 600 tggaggccga catcaatggc ctgcgcaggg tgctggatga gctgaccctg gccagagccg 660 acctggagat gcagattgag aacctcaagg aggagctggc ctacctgaag aagaaccacg 720 aggaggagat gaacgccctg cgaggccagg tgggtggtga gatcaatgtg gagatggacg 780 ctgccccagg cgtggacctg agccgcatcc tcaacgagat gcgtgaccag tatgagaaga 840 tggcagagaa gaaccgcaag gatgccgagg attggttctt cagcaagaca gaggaactga 900 accgcgaggt ggccaccaac agtgagctgg tgcagagtgg caagagtgag atctcggagc 960 tccggcgcac catgcaggcc ttggagatag agctgcagtc ccagctcagc atgaaagcat 1020 ccctggaggg caacctggcg gagacagaga accgctactg cgtgcagctg tcccagatcc 1080 aggggctgat tggcagcgtg gaggagcagc tggcccagct tcgctgcgag atggagcagc 1140 agaaccagga atacaaaatc ctgctggatg tgaagacgcg gctggagcag gagattgcca 1200 cctaccgccg cctgctggag ggagaggatg cccacctgac tcagtacaag aaagaaccgg 1260 tgaccacccg tcaggtgcgt accattgtgg aagaggtcca ggatggcaag gtcatctcct 1320 cccgcgagca ggtccaccag accacccgct gaggactcag ctaccccggc cggccaccca 1380 ggaggcaggg aggcagccgc cccatctgcc ccacagtctc cggcctctcc agcctcagcc 1440 ccctgcttca gtcccttccc catgcttcct tgcctgatga caataaagct tgttgactca 1500 gctaaaaaaa a 1511 9 432 PRT Homo sapiens misc_feature Incyte ID No 1454852CD1 9 Met Thr Thr Ser Ile Arg Gln Phe Thr Ser Ser Ser Ser Ile Lys 1 5 10 15 Gly Ser Ser Gly Leu Gly Gly Gly Ser Ser Arg Thr Ser Cys Arg 20 25 30 Leu Ser Gly Gly Leu Gly Ala Gly Ser Cys Arg Leu Gly Ser Ala 35 40 45 Gly Gly Leu Gly Ser Thr Leu Gly Gly Ser Ser Tyr Ser Ser Cys 50 55 60 Tyr Ser Phe Gly Ser Gly Gly Gly Tyr Gly Ser Ser Phe Gly Gly 65 70 75 Val Asp Gly Leu Leu Ala Gly Gly Glu Lys Ala Thr Met Gln Asn 80 85 90 Leu Asn Asp Arg Leu Ala Ser Tyr Leu Asp Lys Val Arg Ala Leu 95 100 105 Glu Glu Ala Asn Thr Glu Leu Glu Val Lys Ile Arg Asp Trp Tyr 110 115 120 Gln Arg Gln Ala Pro Gly Pro Ala Arg Asp Tyr Ser Gln Tyr Tyr 125 130 135 Arg Thr Ile Glu Glu Leu Gln Asn Lys Ile Leu Thr Ala Thr Val 140 145 150 Asp Asn Ala Asn Ile Leu Leu Gln Ile Asp Asn Ala Arg Leu Ala 155 160 165 Ala Asp Asp Phe Arg Thr Lys Phe Glu Thr Glu Gln Ala Leu Arg 170 175 180 Leu Ser Val Glu Ala Asp Ile Asn Gly Leu Arg Arg Val Leu Asp 185 190 195 Glu Leu Thr Leu Ala Arg Ala Asp Leu Glu Met Gln Ile Glu Asn 200 205 210 Leu Lys Glu Glu Leu Ala Tyr Leu Lys Lys Asn His Glu Glu Glu 215 220 225 Met Asn Ala Leu Arg Gly Gln Val Gly Gly Glu Ile Asn Val Glu 230 235 240 Met Asp Ala Ala Pro Gly Val Asp Leu Ser Arg Ile Leu Asn Glu 245 250 255 Met Arg Asp Gln Tyr Glu Lys Met Ala Glu Lys Asn Arg Lys Asp 260 265 270 Ala Glu Asp Trp Phe Phe Ser Lys Thr Glu Glu Leu Asn Arg Glu 275 280 285 Val Ala Thr Asn Ser Glu Leu Val Gln Ser Gly Lys Ser Glu Ile 290 295 300 Ser Glu Leu Arg Arg Thr Met Gln Ala Leu Glu Ile Glu Leu Gln 305 310 315 Ser Gln Leu Ser Met Lys Ala Ser Leu Glu Gly Asn Leu Ala Glu 320 325 330 Thr Glu Asn Arg Tyr Cys Val Gln Leu Ser Gln Ile Gln Gly Leu 335 340 345 Ile Gly Ser Val Glu Glu Gln Leu Ala Gln Leu Arg Cys Glu Met 350 355 360 Glu Gln Gln Asn Gln Glu Tyr Lys Ile Leu Leu Asp Val Lys Thr 365 370 375 Arg Leu Glu Gln Glu Ile Ala Thr Tyr Arg Arg Leu Leu Glu Gly 380 385 390 Glu Asp Ala His Leu Thr Gln Tyr Lys Lys Glu Pro Val Thr Thr 395 400 405 Arg Gln Val Arg Thr Ile Val Glu Glu Val Gln Asp Gly Lys Val 410 415 420 Ile Ser Ser Arg Glu Gln Val His Gln Thr Thr Arg 425 430 10 309 DNA Homo sapiens misc_feature Incyte ID No 353005.1 10 ggtggntggn accatggnac tgtnnatctc cccctcttcc tcttggcctc tgtggacggt 60 gcctttncat ctgctnccac ttnaatcctc tgtctctnga ggaactaggc tccaacacgg 120 ggatccaggt tttcaatcag attgtgaagt cgaggcctna tgacaacatc gtgatctctc 180 cccatgggat tgcgtcggtc ctggggatgc ttcagctggg ggcggacggc aggaccagaa 240 gcagctcgcc atggtgatga gatacggcgt aaatgatatg attgacaatn tgctgtcccc 300 agatcttat 309 11 176 DNA Homo sapiens misc_feature Incyte ID No 378497.1 11 gcccaacgtc atcgggcngc agtgcacccn ctgtncaana ggancactac gnattcccac 60 gctgcaaccg tgcagctgtg gtcggcncct ttntgaagag atgacggngc antnccggct 120 tcccttcccc gcacggtcag gccccagtgt naggtgtgtg agacanantn cattca 176 12 3544 DNA Homo sapiens misc_feature Incyte ID No 994684.9 12 cagcgtcaaa tttgtctcca ccacctcctc ctcccggaag agcttcaaga gctaagaacc 60 tgctgcaagt cactgccttc caagtgcagc aacccagccc atggagattg cctcttctag 120 gcagttgctc aagccatgtt ttatcctttt ctggatagca tcatcgctga ggtcaaggcc 180 cagtatgagg agattgccaa ccgcagccgg acagaagccg agtcctggta tcagaccaag 240 tatgaggagc tgcagcagac agctggccgg catggcgatg acctccgcaa caccaagcat 300 gagatctctg agatgaaccg gatgatccag aggctgagag ccgagattga caatgtcaag 360 aaacagtgcg ccaatctgca gaacgccatt gcggatgccg agcagcgtgg ggagctggcc 420 ctcaaggatg ccaggaacaa gctggccgag ctggaggagg ccctgcagaa ggccaagcag 480 gacatggccc ggctgctgcg tgagtaccag gagctcatga acaccaagct ggccctggac 540 gtggagatcg ccacttaccg caagctgctg gagggcgagg aatgcagact cagtggagaa 600 ggagttggac cagtcaacat ctgtaagtag ctttgaacag acattaacaa cgacaataat 660 atgggatata tttagtgcca actcagaatt ctgctgtttc tagatccaaa cttttcccat 720 cccagcatat ggttatttat aataatacac ttagtaagtt gtgggtggtg gaggggaagg 780 acagattggg acaggaagca atgtggctta tgtctcatct cttaaagggt aagccatgca 840 tcctatgctt cttggaccct gtcccctgcc ttgtccctag tacctagctc cccccagtac 900 ctagctcctc ccctcagtac ctagctcccc tcagtaccta gctccctgta gtacctagct 960 cccctcagta cctagctcct ctcagtacct agcaccttgc ctcttacact cacccacttt 1020 tttagggacc ttaattaaat gacagttctt ccgggccttg tttgctactc tgtaaagggg 1080 gtccagtaga gtgctccaac accagcagat caaataaatg ggccatgcag gatcagcctg 1140 gcagatggtc tcactgagtc ctccctcctt tccctgcagc tgttgtcaca agcagtgttt 1200 cctctggata tggcagtggc agtggctatg gcggtggcct cggtggaggt cttggcggcg 1260 gcctcggtgg aggtcttgcc ggaggtagca gtggaagcta ctactccagc agcagtgggg 1320 gtgtcggcct aggtggtggg ctcagtgtgg ggggctctgg cttcagtgca agcagtggcc 1380 gagggctggg ggtgggcttt ggcagtggcg ggggtagcag ctccagcgtc aaatttgtct 1440 ccaccacctc ctcctcccgg aagagcttca agagctaaga acctgctgca agtcactgcc 1500 ttccaagtgc agcaacccag cccatggaga ttgcctcttc taggcagagt cagccttgcg 1560 ggtgcttgtg gagtgggtgg ctatggcagc cggagcctct acaacctggg gggctccaag 1620 aggatatcca tcagcactag tggtggcagc ttcaggaacc ggtttggtgc tggtgctgga 1680 ggcggctatg gctttggagg tggtgccggt agtggatttg gtttcggcgg tggagctggt 1740 ggtggctttg ggctcggtgg cggagctggc tttggaggtg gcttcggtgg ccctggcttt 1800 cctgtctgcc ctcctggagg tatccaagag gtcactgtca accagagtct cctgactccc 1860 ctcaacctgc aaatcgaccc cagcatccag agggtgagga ccgaggagcg cgagcagatc 1920 aagaccctca acaataagtt tgcctccttc atcgacaagg tgcggttcct ggagcagcag 1980 aacaaggttc tggaaacaaa gtggaccctg ctgcaggagc agggcaccaa gactgtgagg 2040 cagaacctgg agccgttgtt cgagcagtac atcaacaacc tcaggaggca gctggacagc 2100 atcgtggggg aacggggccg cctggactca gagctgagaa acatgcagga cctggtggaa 2160 gacttcaaga acaagtatga ggatgaaatc aacaagcgta ccactgctga gaatgagttt 2220 gtgatgctga agaaggatgt agatgctgcc tacatgaaca aggtggagct ggaggccaag 2280 gttgatgcac tgatggatga gattaacttc atgaagatgt tctttgatgc ggagctgtcc 2340 cagatgcaga cgcatgtctc tgacacctca gtggtcctct ccatggacaa caaccgcaac 2400 ctggacctgg atagcatcat cgctgaggtc aaggcccagt atgaggagat tgccaaccgc 2460 agccggaccg aagccgagtc ctggtatcag accaagtatg aggagctgca gcagacagct 2520 ggccggcatg gcgatgacct ccgcaacacc aagcatgaga tctctgagat gaaccggatg 2580 atccagaggc tgagagccga gattgacaat gtcaagaaac agtgcgccaa tctggcagaa 2640 cgccattgcg gatgccgagc agcgtgggga gctggccctc aaggatgcca ggaacaagct 2700 ggccgagctg gaggaggccc tgcagaaggc caagcaggac atgggcccgg ctgctgcgtg 2760 agtaccagga gctcatgaac accaagctgg ccctggacgt ggagatcgcc acttaccgca 2820 agctgctgga gggcgaggaa tgcagactca gtggagaagg agttggacca gtcaacatct 2880 ctgttgtcac aagcagtgtt tcctctggat atggcagtgg cagtggctat ggcggtggcc 2940 tcggtggagg tcttggcggc ggcctcggtg gaggtcttgc cggaggtagc agtggaagct 3000 actactccag cagcagtggg ggtgtcggcc taggtggtgg gctcagtgtg gggggctctg 3060 gcttcagtgc aagcagtggc cgagggctgg gggtgggctt tggcagtggc gggggtagca 3120 gctccagcgt caaatttgtc tccaccacct cctcctcccg gaagagcttc aagagctaag 3180 aacctgctgc aagtcactgc cttccaagtg cagcaaccca gcccatggag attgcctctt 3240 ctaggcagtt gctcaagcca tgttttatcc ttttctggag agtagtctag accaagccaa 3300 ttgcagaacc acattctttg gttcccagga gagccccatt cccagcccct ggtctcccgt 3360 gccgcagttc tatattctgc ttcaaatcag ccttcaggtt tcccacagca tggcccctgc 3420 tgacacgaga acccaaagtt ttcccaaatc taaatcatca aaacagaatc cccaccccaa 3480 tcccaaattt tgttttggtt ctaactacct ccagaatgtg ttcaataaaa tgcttttata 3540 ttat 3544 13 3000 DNA Homo sapiens misc_feature Incyte ID No 995610.1 13 ggagtttatt cataacgcgc tctccaagta tacgtggcaa tgcgttgctg ggttatttta 60 atcattctag gcatcgtttt cctccttatg cctctatcat tcctccctat ctacactaac 120 atcccacgct ctgaacgcgc gcccattaat acccttcttt cctccactct ccctgggact 180 cttgatcaaa gcgcggccct ttccccagcc ttagcgaggc gccctgcagc ctggtacgcg 240 cgtggcgtgg cggtgggcgc gcagtgcgtt ctcggtgtgg agggcagctg ttccgcctgc 300 gatgatttat actcacagga caaggatgcg gtttgtcaaa cagtactgct acggaggagc 360 agcagagaaa gggagagggt ttgagaggga gcaaaagaaa atggtaggcg cgcgtagtta 420 attcatgcgg ctctcttact ctgtttacat cctagagcta gagtgctcgg ctgcccggct 480 gagtctcctc cccaccttcc ccaccctccc caccctcccc ataagcgccc tcccgggttc 540 ccaaagcaga gggcgtgggg gaaaagaaaa aagatcctct ctcgctaatc tccgcccacc 600 ggccctttat aatgcgaggg tctggacggc tgaggacccc cgagctgtgc tgctcgcggc 660 cgccaccgcc gggccccggc cgtccctggc tcccctcctg cctcgagaag ggcagggctt 720 ctcagaggct tggcgggaaa aagaacggag ggagggatcg cgctgagtat aaaagccggt 780 tttcggggct ttatctaact cgctgtagta attccagcga gaggcagagg gagcgagcgg 840 gcggccggct agggtggaag agccgggcga gcagagctgc gctgcgggcg tcctgggaag 900 ggagatccgg agcgaatagg gggcttcgcc tctggcccag ccctcccgct gatcccccag 960 ccagcggtcc gcaacccttg ccgcatccac gaaactttgc ccatagcagc gggcgggcac 1020 tttgcactgg aacttacaac acccgagcaa ggacgcgact ctcccgacgc ggggaggcta 1080 ttctgcccat ttggggacac ttccccgccg ctgccaggac ccgcttctct gaaaggctct 1140 ccttgcagct gcttagacgc tggatttttt tcgggtagtg gaaaaccagc agcctcccgc 1200 gacgatgccc ctcaacgtta gcttcaccaa caggaactat gacctcgact acgactcggt 1260 gcagccgtat ttctactgcg acgaggagga gaacttctac cagcagcagc agcagagcga 1320 ggctgcagcc cccggcgccc agcgaggata tctggaagaa attcgagctg ctgcccaccc 1380 cgcccctgtc ccctagccgc cgctccgggc tctgctcgcc ctcctacgtt gcggtcacac 1440 ccttctccct tcggggagac aacgacggcg gtggcgggag cttctccacg gccgaccagc 1500 tggagatggt gaccgagctg ctgggaggag acatggtgaa ccagagtttc atctgcgacc 1560 cggacgacga gaccttcatc aaaaacatca tcatccagga ctgtatgtgg agcggcttct 1620 cggccgccgc caagctcgtc tcagagaagc tggcctccta ccaggctgcg cgcaaagaca 1680 gcggcagccc gaaccccgcc cgcggccaca gcgtctgctc cacctccagc ttgtacctgc 1740 aggatctgag cgccgccgcc tcagagtgca tcgacccctc ggtggtcttc ccctaccctc 1800 tcaacgacag cagctcgccc aagtcctgcg cctcgcaaga ctccagcgcc ttctctccgt 1860 cctcggattc tctgctctcc tcgacggagt cctccccgca gggcagcccc gagcccctgg 1920 tgctccatga ggagacaccg cccaccacca gcagcgactc tgaggaggaa caagaagatg 1980 aggaagaaat cgatgttgtt tctgtggaaa agaggcaggc tcctggcaaa aggtcagagt 2040 ctggatcacc ttctgctgga ggccacagca aacctcctca cagcccactg gtcctcaaga 2100 ggtgccacgt ctccacacat cagcacaact acgcagcgcc tccctccact cggaaggact 2160 atcctgctgc caagagggtc aagttggaca gtgtcagagt cctgagacag atcagcaaca 2220 accgaaaatg caccagcccc aggtcctcgg acaccgagga gaatgtcaag aggcgaacac 2280 acaacgtctt ggagcgccag aggaggaacg agctaaaacg gagctttttt gccctgcgtg 2340 accagatccc ggagttggaa aacaatgaaa aggcccccaa ggtagttatc cttaaaaaag 2400 ccacagcata catcctgtcc gtccaagcag aggagcaaaa gctcatttct gaagaggact 2460 tgttgcggaa acgacgagaa cagttgaaac acaaacttga acagctacgg aactcttgtg 2520 cgtaaggaaa agtaaggaaa acgattcctt ctaacagaaa tgtcctgagc aatcacctat 2580 gaacttgttt caaatgcatg atcaaatgca acctcacaac cttggctgag tcttgagact 2640 gaaagattta gccataatgt aaactgcctc aaattggact ttgggcataa aagaactttt 2700 ttatgcttac catctttttt ttttctttaa cagatttgta tttaagaatt gtttttaaaa 2760 aattttaaga tttacacaat gtttctctgt aaatattgcc attaaatgta aataacttta 2820 ataaaacgtt tatagcagtt acacagaatt tcaatcctag tatatagtac ctagtattat 2880 aggtactata aaccctaatt ttttttattt aagtacattt tgctttttaa agttgatttt 2940 tttctattgt ttttagaaaa aataaaataa ctggcaaata tatcattgag ccaaaaaaaa 3000 14 427 DNA Homo sapiens misc_feature Incyte ID No 417119.1 14 aaaacaaaga aggctggaaa ccaaagcaat catctcttta gtggaaacta ttcttaaaga 60 agatcttgat ggctactgac atttgcaact ccctcactct ttctcagggg cctttcactt 120 acattgtcac cagaggttcg taacctccct gtgggctagt gttatgacca tcaccatttt 180 acctaagtag ctctgttgct cggccacagt gagcagtaat agacctgaag ctggaaccca 240 tgtctaatag tgtcaggtcc agtgttctta gccaccccac tcccagcttc atccctactg 300 gtgttgtcat cagactttga ccgtatatgc tcaggtgtcc tccaagaaat caaattttgc 360 cacctcgcct tcacgaggcc tgcccttctg gatttatacc taacaacatg tgctccacat 420 ttcagaa 427 15 4108 DNA Homo sapiens misc_feature Incyte ID No 3615080CB1 15 tgccagattc ctgagacccg cctgcggtgg ggctacaccc agccagggag tctccagagg 60 tgaggctgtt gtttaaaaac ctggagccgg gaggggagac ccccacattc aagaggagct 120 ttcaggcgat ctggagaaag aacggcagaa cacacagcaa ggaaaggtcc tttctgggga 180 tcaccccatt ggctgaagat gagaccattc ttcctcttgt gttttgccct gcctggcctc 240 ctgcatgccc aacaagcctg ctcccgtggg gcctgctatc cacctgttgg ggacctgctt 300 gttgggagga cccggtttct ccgagcttca tctacctgtg gactgaccaa gcctgagacc 360 tactgcaccc agtatggcga gtggcagatg aaatgctgca agtgtgactc caggcagcct 420 cacaactact acagtcaccg agtagagaat gtggcttcat cctccggccc catgcgctgg 480 tggcagtcac agaatgatgt gaaccctgtc tctctgcagc tggacctgga caggagattc 540 cagcttcaag aagtcatgat ggagttccag gggcccatgc ccgccggcat gctgattgag 600 cgctcctcag acttcggtaa gacctggcga gtgtaccagt acctggctgc cgactgcacc 660 tccaccttcc ctcgggtccg ccagggtcgg cctcagagct ggcaggatgt tcggtgccag 720 tccctgcctc agaggcctga tgcacgccta aatgggggga aggtccaact taaccttatg 780 gatttagtgt ctgggattcc agcaactcaa agtcaaaaaa ttcaagaggt gggggagatc 840 acaaacttga gagtcaattt caccaggctg gcccctgtgc cccaaagggg ctaccaccct 900 cccagcgcct actatgctgt gtcccagctc cgtctgcagg ggagctgctt ctgtcacggc 960 catgctgatc gctgcgcacc caagcctggg gcctctgcag gcccctccac cgctgtgcag 1020 gtccacgatg tctgtgtctg ccagcacaac actgccggcc caaattgtga gcgctgtgca 1080 cccttctaca acaaccggcc ctggagaccg gcggagggcc aggacgccca tgaatgccaa 1140 aggtgcgact gcaatgggca ctcagagaca tgtcactttg accccgctgt gtttgccgcc 1200 agccaggggg catatggagg tgtgtgtgac aattgccggg accacaccga aggcaagaac 1260 tgtgagcggt gtcagctgca ctatttccgg aaccggcgcc cgggagcttc cattcaggag 1320 acctgcatct cctgcgagtg tgatccggat ggggcagtgc caggggctcc ctgtgaccca 1380 gtgaccgggc agtgtgtgtg caaggagcat gtgcagggag agcgctgtga cctatgcaag 1440 ccgggcttca ctggactcac ctacgccaac ccgcagggct gccaccgctg tgactgcaac 1500 atcctggggt cccggaggga catgccgtgt gacgaggaga gtgggcgctg cctttgtctg 1560 cccaacgtgg tgggtcccaa atgtgaccag tgtgctccct accactggaa gctggccagt 1620 ggccagggct gtgaaccgtg tgcctgcgac ccgcacaact ccctcagccc acagtgcaac 1680 cagttcacag ggcagtgccc ctgtcgggaa ggctttggtg gcctgatgtg cagcgctgca 1740 gccatccgcc agtgtccaga ccggacctat ggagacgtgg ccacaggatg ccgagcctgt 1800 gactgtgatt tccggggaac agagggcccg ggctgcgaca aggcatcagg ccgctgcctc 1860 tgccgccctg gcttgaccgg gccccgctgt gaccagtgcc agcgaggcta ctgcaatcgc 1920 tacccggtgt gcgtggcctg ccacccttgc ttccagacct atgatgcgga cctccgggag 1980 caggccctgc gctttggtag actccgcaat gccaccgcca gcctgtggtc agggcctggg 2040 ctggaggacc gtggcctggc ctcccggatc ctagatgcaa agagtaagat tgagcagatc 2100 cgagcagttc tcagcagccc cgcagtcaca gagcaggagg tggctcaggt ggccagtgcc 2160 atcctctccc tcaggcgaac tctccagggc ctgcagctgg atctgcccct ggaggaggag 2220 acgttgtccc ttccgagaga cctggagagt cttgacagaa gcttcaatgg tctccttact 2280 atgtatcaga ggaagaggga gcagtttgaa aaaataagca gtgctgatcc ttcaggagcc 2340 ttccggatgc tgagcacagc ctacgagcag tcagcccagg ctgctcagca ggtctccgac 2400 agctcgcgcc ttttggacca gctcagggac agccggagag aggcagagag gctggtgcgg 2460 caggcgggag gaggaggagg caccggcagc cccaagcttg tggccctgag gctggagatg 2520 tcttcgttgc ctgacctgac acccaccttc aacaagctct gtggcaactc caggcagatg 2580 gcttgcaccc caatatcatg ccctggtgag ctatgtcccc aagacaatgg cacagcctgt 2640 ggctcccgct gcaggggtgt ccttcccagg gccggtgggg ccttcttgat ggcggggcag 2700 gtggctgagc agctgcgggg cttcaatgcc cagctccagc ggaccaggca gatgattagg 2760 gcagccgagg aatctgcctc acagattcaa tccagtgccc agcgcttgga gacccaggtg 2820 agcgccagcc gctcccagat ggaggaagat gtcagacgca cacggctcct aatccagcag 2880 gtccgggact tcctaacaga ccccgacact gatgcagcca ctatccagga ggtcagcgag 2940 gccgtgctgg ccctgtggct gcccacagac tcagatactg ttctgcagaa gatgaatgag 3000 atccaggcca ttgcagccag gctccccaac gtggacttgg tgctgtccca gaccaagcag 3060 gacattgcgc gtgcccgccg gttgcaggct gaggctgagg aagccaggag ccgagcccat 3120 gcagtggagg gccaggtgga agatgtggtt gggaacctgc ggcaggggac agtggcactg 3180 caggaagctc aggacaccat gcaaggcacc agccgctccc ttcggcttat ccaggacagg 3240 gttgctgagg ttcagcaggt actgcggcca gcagaaaagc tggtgacaag catgaccaag 3300 cagctgggtg acttctggac acggatggag gagctccgcc accaagcccg gcagcagggg 3360 gcagaggcag tccaggccca gcagcttgcg gaaggtgcca gcgagcaggc attgagtgcc 3420 caagagggat ttgagagaat aaaacaaaag tatgctgagt tgaaggaccg gttgggtcag 3480 agttccatgc tgggtgagca gggtgcccgg atccagagtg tgaagacaga ggcagaggag 3540 ctgtttgggg agaccatgga gatgatggac aggatgaaag acatggagtt ggagctgctg 3600 cggggcagcc aggccatcat gctgcgctca gcggacctga caggactgga gaagcgtgtg 3660 gagcagatcc gtgaccacat caatgggcgc gtgctctact atgccacctg caagtgatgc 3720 tacagcttcc agcccgttgc cccactcatc tgccgccttt gcttttggtt gggggcagat 3780 tgggttggaa tgctttccat ctccaggaga ctttcatgta gcctaaagta cagcctggac 3840 cacccctggt gtgtagctag taagattacc ctgagctgca gctgagcctg agccaatggg 3900 acagttacac ttgacagaca aagatggtgg agattggcat gccattgaaa ctaagagctc 3960 tcaagtcaag gaagctgggc tgggcagtat cccccgcctt tagttctcca ctggggagga 4020 atcctggacc aagcacaaaa acttaacaaa agtgatgtaa aaatgaaaag ccaaataaaa 4080 atctttggaa aagaaaaaaa aaaaaaaa 4108 16 1172 PRT Homo sapiens misc_feature Incyte ID No 3615080CD1 16 Met Arg Pro Phe Phe Leu Leu Cys Phe Ala Leu Pro Gly Leu Leu 1 5 10 15 His Ala Gln Gln Ala Cys Ser Arg Gly Ala Cys Tyr Pro Pro Val 20 25 30 Gly Asp Leu Leu Val Gly Arg Thr Arg Phe Leu Arg Ala Ser Ser 35 40 45 Thr Cys Gly Leu Thr Lys Pro Glu Thr Tyr Cys Thr Gln Tyr Gly 50 55 60 Glu Trp Gln Met Lys Cys Cys Lys Cys Asp Ser Arg Gln Pro His 65 70 75 Asn Tyr Tyr Ser His Arg Val Glu Asn Val Ala Ser Ser Ser Gly 80 85 90 Pro Met Arg Trp Trp Gln Ser Gln Asn Asp Val Asn Pro Val Ser 95 100 105 Leu Gln Leu Asp Leu Asp Arg Arg Phe Gln Leu Gln Glu Val Met 110 115 120 Met Glu Phe Gln Gly Pro Met Pro Ala Gly Met Leu Ile Glu Arg 125 130 135 Ser Ser Asp Phe Gly Lys Thr Trp Arg Val Tyr Gln Tyr Leu Ala 140 145 150 Ala Asp Cys Thr Ser Thr Phe Pro Arg Val Arg Gln Gly Arg Pro 155 160 165 Gln Ser Trp Gln Asp Val Arg Cys Gln Ser Leu Pro Gln Arg Pro 170 175 180 Asp Ala Arg Leu Asn Gly Gly Lys Val Gln Leu Asn Leu Met Asp 185 190 195 Leu Val Ser Gly Ile Pro Ala Thr Gln Ser Gln Lys Ile Gln Glu 200 205 210 Val Gly Glu Ile Thr Asn Leu Arg Val Asn Phe Thr Arg Leu Ala 215 220 225 Pro Val Pro Gln Arg Gly Tyr His Pro Pro Ser Ala Tyr Tyr Ala 230 235 240 Val Ser Gln Leu Arg Leu Gln Gly Ser Cys Phe Cys His Gly His 245 250 255 Ala Asp Arg Cys Ala Pro Lys Pro Gly Ala Ser Ala Gly Pro Ser 260 265 270 Thr Ala Val Gln Val His Asp Val Cys Val Cys Gln His Asn Thr 275 280 285 Ala Gly Pro Asn Cys Glu Arg Cys Ala Pro Phe Tyr Asn Asn Arg 290 295 300 Pro Trp Arg Pro Ala Glu Gly Gln Asp Ala His Glu Cys Gln Arg 305 310 315 Cys Asp Cys Asn Gly His Ser Glu Thr Cys His Phe Asp Pro Ala 320 325 330 Val Phe Ala Ala Ser Gln Gly Ala Tyr Gly Gly Val Cys Asp Asn 335 340 345 Cys Arg Asp His Thr Glu Gly Lys Asn Cys Glu Arg Cys Gln Leu 350 355 360 His Tyr Phe Arg Asn Arg Arg Pro Gly Ala Ser Ile Gln Glu Thr 365 370 375 Cys Ile Ser Cys Glu Cys Asp Pro Asp Gly Ala Val Pro Gly Ala 380 385 390 Pro Cys Asp Pro Val Thr Gly Gln Cys Val Cys Lys Glu His Val 395 400 405 Gln Gly Glu Arg Cys Asp Leu Cys Lys Pro Gly Phe Thr Gly Leu 410 415 420 Thr Tyr Ala Asn Pro Gln Gly Cys His Arg Cys Asp Cys Asn Ile 425 430 435 Leu Gly Ser Arg Arg Asp Met Pro Cys Asp Glu Glu Ser Gly Arg 440 445 450 Cys Leu Cys Leu Pro Asn Val Val Gly Pro Lys Cys Asp Gln Cys 455 460 465 Ala Pro Tyr His Trp Lys Leu Ala Ser Gly Gln Gly Cys Glu Pro 470 475 480 Cys Ala Cys Asp Pro His Asn Ser Leu Ser Pro Gln Cys Asn Gln 485 490 495 Phe Thr Gly Gln Cys Pro Cys Arg Glu Gly Phe Gly Gly Leu Met 500 505 510 Cys Ser Ala Ala Ala Ile Arg Gln Cys Pro Asp Arg Thr Tyr Gly 515 520 525 Asp Val Ala Thr Gly Cys Arg Ala Cys Asp Cys Asp Phe Arg Gly 530 535 540 Thr Glu Gly Pro Gly Cys Asp Lys Ala Ser Gly Arg Cys Leu Cys 545 550 555 Arg Pro Gly Leu Thr Gly Pro Arg Cys Asp Gln Cys Gln Arg Gly 560 565 570 Tyr Cys Asn Arg Tyr Pro Val Cys Val Ala Cys His Pro Cys Phe 575 580 585 Gln Thr Tyr Asp Ala Asp Leu Arg Glu Gln Ala Leu Arg Phe Gly 590 595 600 Arg Leu Arg Asn Ala Thr Ala Ser Leu Trp Ser Gly Pro Gly Leu 605 610 615 Glu Asp Arg Gly Leu Ala Ser Arg Ile Leu Asp Ala Lys Ser Lys 620 625 630 Ile Glu Gln Ile Arg Ala Val Leu Ser Ser Pro Ala Val Thr Glu 635 640 645 Gln Glu Val Ala Gln Val Ala Ser Ala Ile Leu Ser Leu Arg Arg 650 655 660 Thr Leu Gln Gly Leu Gln Leu Asp Leu Pro Leu Glu Glu Glu Thr 665 670 675 Leu Ser Leu Pro Arg Asp Leu Glu Ser Leu Asp Arg Ser Phe Asn 680 685 690 Gly Leu Leu Thr Met Tyr Gln Arg Lys Arg Glu Gln Phe Glu Lys 695 700 705 Ile Ser Ser Ala Asp Pro Ser Gly Ala Phe Arg Met Leu Ser Thr 710 715 720 Ala Tyr Glu Gln Ser Ala Gln Ala Ala Gln Gln Val Ser Asp Ser 725 730 735 Ser Arg Leu Leu Asp Gln Leu Arg Asp Ser Arg Arg Glu Ala Glu 740 745 750 Arg Leu Val Arg Gln Ala Gly Gly Gly Gly Gly Thr Gly Ser Pro 755 760 765 Lys Leu Val Ala Leu Arg Leu Glu Met Ser Ser Leu Pro Asp Leu 770 775 780 Thr Pro Thr Phe Asn Lys Leu Cys Gly Asn Ser Arg Gln Met Ala 785 790 795 Cys Thr Pro Ile Ser Cys Pro Gly Glu Leu Cys Pro Gln Asp Asn 800 805 810 Gly Thr Ala Cys Gly Ser Arg Cys Arg Gly Val Leu Pro Arg Ala 815 820 825 Gly Gly Ala Phe Leu Met Ala Gly Gln Val Ala Glu Gln Leu Arg 830 835 840 Gly Phe Asn Ala Gln Leu Gln Arg Thr Arg Gln Met Ile Arg Ala 845 850 855 Ala Glu Glu Ser Ala Ser Gln Ile Gln Ser Ser Ala Gln Arg Leu 860 865 870 Glu Thr Gln Val Ser Ala Ser Arg Ser Gln Met Glu Glu Asp Val 875 880 885 Arg Arg Thr Arg Leu Leu Ile Gln Gln Val Arg Asp Phe Leu Thr 890 895 900 Asp Pro Asp Thr Asp Ala Ala Thr Ile Gln Glu Val Ser Glu Ala 905 910 915 Val Leu Ala Leu Trp Leu Pro Thr Asp Ser Asp Thr Val Leu Gln 920 925 930 Lys Met Asn Glu Ile Gln Ala Ile Ala Ala Arg Leu Pro Asn Val 935 940 945 Asp Leu Val Leu Ser Gln Thr Lys Gln Asp Ile Ala Arg Ala Arg 950 955 960 Arg Leu Gln Ala Glu Ala Glu Glu Ala Arg Ser Arg Ala His Ala 965 970 975 Val Glu Gly Gln Val Glu Asp Val Val Gly Asn Leu Arg Gln Gly 980 985 990 Thr Val Ala Leu Gln Glu Ala Gln Asp Thr Met Gln Gly Thr Ser 995 1000 1005 Arg Ser Leu Arg Leu Ile Gln Asp Arg Val Ala Glu Val Gln Gln 1010 1015 1020 Val Leu Arg Pro Ala Glu Lys Leu Val Thr Ser Met Thr Lys Gln 1025 1030 1035 Leu Gly Asp Phe Trp Thr Arg Met Glu Glu Leu Arg His Gln Ala 1040 1045 1050 Arg Gln Gln Gly Ala Glu Ala Val Gln Ala Gln Gln Leu Ala Glu 1055 1060 1065 Gly Ala Ser Glu Gln Ala Leu Ser Ala Gln Glu Gly Phe Glu Arg 1070 1075 1080 Ile Lys Gln Lys Tyr Ala Glu Leu Lys Asp Arg Leu Gly Gln Ser 1085 1090 1095 Ser Met Leu Gly Glu Gln Gly Ala Arg Ile Gln Ser Val Lys Thr 1100 1105 1110 Glu Ala Glu Glu Leu Phe Gly Glu Thr Met Glu Met Met Asp Arg 1115 1120 1125 Met Lys Asp Met Glu Leu Glu Leu Leu Arg Gly Ser Gln Ala Ile 1130 1135 1140 Met Leu Arg Ser Ala Asp Leu Thr Gly Leu Glu Lys Arg Val Glu 1145 1150 1155 Gln Ile Arg Asp His Ile Asn Gly Arg Val Leu Tyr Tyr Ala Thr 1160 1165 1170 Cys Lys 17 795 DNA Homo sapiens misc_feature Incyte ID No 331749.3 17 attttacata cactgtatgt tatagaactt catggatcag atctggggca gcaccctata 60 aatcaccacc ttaatatgct gcaacaaaat gtagaatatt cagacaaaat ggatacataa 120 agactaagta gcccataagg ggtcaaattt tgctgccaaa tgcgtatgcc accaacttac 180 aaaaacactt cgttcgcaga gcttttcaga ttgtggaatg ttggataagg aattatagac 240 ctctagtagc tgaaatgcaa gaccccaaga ggaagttcag atcttaatat aaattcactt 300 tcatttttga tagctgtccc atctggtcat ttggttggca ctagactggt ggcaggggct 360 tctagctgac tcgcacaggg attctcacaa tagccgatat cagaatttgt gttgaaggaa 420 cttgtctctt catctaatat gatagcggga aaaggagagg aaactactgc ctttagaaaa 480 tataagtaaa gtgattaaag tgctcacgtt accttgacac atagtttttc agtctatggg 540 tttagttact ttagatggca agcatgtaac ttatattaat agtaatttgt aaagttggtt 600 ggataagcta tccatgttgc aggttcatgg attacttctc tataaaaaat atgtatttac 660 caaaaaattt tgtgacattc cttctcccat ctcttccttg acatgcattg taaataggtt 720 cttcttgttc tgagattcaa tattgaattt ctcctatgct attgacaata aaatattatt 780 gaactacaaa aaaaa 795 18 2538 DNA Homo sapiens misc_feature Incyte ID No 979243.1 18 cgccaggaca tgcagcccac catgaagttc gtgatggaca catctaaata ctggtttaag 60 ccaaacatca cccgagagca agcaatcgag ctgctgagga aggaggagcc aggggctttg 120 tcataaggga cagctcttca taccgaggct ccttcggcct ggccctgaag gtgcaggagg 180 ttcccgcgtc tgctcagaat cgaccaggtg aggacagcaa tgacctcatc cgacacttcc 240 tcatcgagtc gtctgccaaa ggagtgcatc tcaaaggagc agatgaggag ccctactttg 300 aactgggagg tgcagatggg gcctcggact ctacagacag cccagcctcc tgccagaaga 360 aatctgcggg ctgccacacc ctgtacctga gctcagtgag cgtggagacc ctgactggag 420 ccctggccgt gcagaaagcc atctccacca cctttgagag ggacatcctc cccacgccca 480 ccgtggtcca cttcaaagtc acagagcagg gcatcactct gactgatgtc cagaggaagg 540 tgtttttccg gcgccattac ccactcacca ccctccgctt ctgtggtatg gaccctgagc 600 aacggaagtg gcagaagtac tgcaaaccct cctggatctt tgggtttgtg gccaagagcc 660 agacagagcc tcaggagaac gtatgccacc tctttgcgga gtatgacatg gtccagccag 720 cctcgcaggt catcggcctg gtgactgctc tgctgcagga cgcagaaagg atgtagggga 780 gagactgcct gtgcacctaa ccaacacctc caggggctcg ctaaggagcc cccctccacc 840 ccctgaatgg gtgtggcttg tggccatatt gacagaccaa tctatgggac tagggggatt 900 ggcatcaagt tgacaccctt gaacctgcta tggccttcag cagtcaccat catccagacc 960 ccccgggcct cagtttcctc aatcatagaa gaagaccaat agacaagatc agctgttctt 1020 agatgctggt gggcatttga acatgctcct ccatgattct gaagcatgca cacctctgaa 1080 gacccctgca tgaaaataac ctccaaggac cctctgaccc catcgacctg ggccctgccc 1140 acacaacagt ctgagcaaga gacctgcagc ccctgtttcg tggcagacag caggtgcctg 1200 gcggtgaccc acggggctcc tggcttgcag ctggtgatgg tcaagaactg actacaaaac 1260 aggaatggat agactctatt tccttccata tctgttcctc tgttcctttt cccactttct 1320 gggtggcttt ttgggtccac ccagccagga tgctgcaggc caagctgggt gtggtattta 1380 gggcagctca gcagggggaa cttgtcccca tggtcagagg agacccagct gtcctgcacc 1440 cccttgcaga tgagtatcac cccatctttt ctttccacnn nnnnnnnnnn nnnnnnnnnn 1500 nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn 1560 nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn 1620 nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn 1680 nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn 1740 nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnccattc cttgataggc 1800 gagtattcca aagctggtat cgtagctgcc ctaatgttgc atattaggcg gcgggggcag 1860 agataagggc catctctctg tgattctgcc tcagctcctg tcttgctgag ccctccccca 1920 acccacgctc cannnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn 1980 nnnnnnnnnn nnnnnnnnnn gnccctctac tgctatgtgg cttcaaccag cctcacagcc 2040 acacggggga agcagagagt caagaatgca aagaggccgc ttccctaaga ggcttggagg 2100 agctgggctc tatcccacac ccacccccac cccaccccca cccagcctcc agaagctgga 2160 accatttctc ccgcaggcct gagttcctaa ggaaaccacc ctaccggggt ggaagggagg 2220 gtcagggaag aaacccactc ttgctctacg aggagcaagt gcctgccccc tcccagcagc 2280 cagccctgcc aaagttgcat tatctttggc caaggctggg cctgacggtt atgatttcag 2340 ccctgggcct gcaggagagg ctgagaccag cccacccagc cagtggtcga gcactgcccc 2400 gccgccaaag tctgcagaat gtgagatgag gttctcaagg tcacaggccc cagtcccagc 2460 ctgggggctg gcagaggccc ccatatactc tgctacagct cctatcatga aaaataaaat 2520 gtttgtcttt gcaaaaca 2538 19 1730 DNA Homo sapiens misc_feature Incyte ID No 3189059CB1 19 gcggccgcgc ggtatcccac ccagcccacc ccgccccggc cgacggctga cagctgacct 60 ggatccttcg agcgcccgcc gaccgccagc gatcttccct catcttccgg gctggtttct 120 gctgcgcgag gagcgtgccc tcgccgcccc tctcgccgga cccccggccc ccgatggctc 180 ggatggggct tgcgggcgcc gctggacgct ggtggggact cgctctcggc ttgaccgcat 240 tcttcctccc aggcgtccac tcccaggtgg tccaggtgaa cgactccatg tatggcttca 300 tcggcacaga cgtggttctg cactgcagct ttgccaaccc gcttcccagc gtgaagatca 360 cccaggtcac atggcagaag tccaccaatg gctccaagca gaacgtggcc atctacaacc 420 catccatggg cgtgtccgtg ctggctccct accgcgagcg tgtggaattc ctgcggccct 480 ccttcaccga tggcactatc cgcctctccc gcctggagct ggaggatgag ggtgtctaca 540 tctgcgagtt tgctaccttc cctacgggca atcgagaaag ccagctcaat ctcacggtga 600 tggccaaacc caccaattgg atagagggta cccaggcagt gcttcgagcc aagaaggggc 660 aggatgacaa ggtcctggtg gccacctgca cctcagccaa tgggaagcct cccagtgtgg 720 tatcctggga aactcggtta aaaggtgagg ccagagtacc aggagactcc ggaaccccaa 780 tggcaccagt gacggtcatc agccgctacc gcctggtgcc cagcagggaa gcccaccagc 840 agtccttggc ctgcatcgtc aactaccaca tggaccgctt caaggaaagc ctcactctca 900 acgtgcagta tgagcctgag gtaaccattg aggggtttga tggcaactgg tacctgcagc 960 ggatggacgt gaagctcacc tgcaaagctg atgctaaccc cccagccact gagtaccact 1020 ggaccacgct aaatggctct ctccccaagg gtgtggaggc ccagaacaga accctcttct 1080 tcaagggacc catcaactac agcctggcag ggacctacat ctgtgaggcc accaacccca 1140 tcggtacacg ctcaggccag gtggaggtca atatcacaga attcccctac accccgtctc 1200 ctcccgaaca tgggcggcgc gccgggccgg tgcccacggc catcattggg ggcgtggcgg 1260 ggagcatcct gctggtgttg attgtggtcg gcgggatcgt ggtcgccctg cgtcggcgcc 1320 ggcacacctt caagggtgac tacagcacca agaagcacgt gtatggcaac ggctacagca 1380 aggcaggcat cccccagcac cacccaccaa tggcacagaa cctgcagtac cccgacgact 1440 cagacgacga gaagaaggcc ggcccactgg gtggaagcag ctatgaggag gaggaggagg 1500 aggaggaggg cggtggaggg ggcgagcgca aggtgggcgg cccccacccc aaatatgacg 1560 aggacgccaa gcggccctac ttcaccgtgg atgaggccga ggcccgtcag gacggctacg 1620 gggaccggac tctgggctac cagtacgacc ctgagcagct ggacttggct gagaacatgg 1680 tttctcagaa cgacgggtct ttcatttcca agaaggagtg gtacgtgtag 1730 20 518 PRT Homo sapiens misc_feature Incyte ID No 3189059CD1 20 Met Ala Arg Met Gly Leu Ala Gly Ala Ala Gly Arg Trp Trp Gly 1 5 10 15 Leu Ala Leu Gly Leu Thr Ala Phe Phe Leu Pro Gly Val His Ser 20 25 30 Gln Val Val Gln Val Asn Asp Ser Met Tyr Gly Phe Ile Gly Thr 35 40 45 Asp Val Val Leu His Cys Ser Phe Ala Asn Pro Leu Pro Ser Val 50 55 60 Lys Ile Thr Gln Val Thr Trp Gln Lys Ser Thr Asn Gly Ser Lys 65 70 75 Gln Asn Val Ala Ile Tyr Asn Pro Ser Met Gly Val Ser Val Leu 80 85 90 Ala Pro Tyr Arg Glu Arg Val Glu Phe Leu Arg Pro Ser Phe Thr 95 100 105 Asp Gly Thr Ile Arg Leu Ser Arg Leu Glu Leu Glu Asp Glu Gly 110 115 120 Val Tyr Ile Cys Glu Phe Ala Thr Phe Pro Thr Gly Asn Arg Glu 125 130 135 Ser Gln Leu Asn Leu Thr Val Met Ala Lys Pro Thr Asn Trp Ile 140 145 150 Glu Gly Thr Gln Ala Val Leu Arg Ala Lys Lys Gly Gln Asp Asp 155 160 165 Lys Val Leu Val Ala Thr Cys Thr Ser Ala Asn Gly Lys Pro Pro 170 175 180 Ser Val Val Ser Trp Glu Thr Arg Leu Lys Gly Glu Ala Arg Val 185 190 195 Pro Gly Asp Ser Gly Thr Pro Met Ala Pro Val Thr Val Ile Ser 200 205 210 Arg Tyr Arg Leu Val Pro Ser Arg Glu Ala His Gln Gln Ser Leu 215 220 225 Ala Cys Ile Val Asn Tyr His Met Asp Arg Phe Lys Glu Ser Leu 230 235 240 Thr Leu Asn Val Gln Tyr Glu Pro Glu Val Thr Ile Glu Gly Phe 245 250 255 Asp Gly Asn Trp Tyr Leu Gln Arg Met Asp Val Lys Leu Thr Cys 260 265 270 Lys Ala Asp Ala Asn Pro Pro Ala Thr Glu Tyr His Trp Thr Thr 275 280 285 Leu Asn Gly Ser Leu Pro Lys Gly Val Glu Ala Gln Asn Arg Thr 290 295 300 Leu Phe Phe Lys Gly Pro Ile Asn Tyr Ser Leu Ala Gly Thr Tyr 305 310 315 Ile Cys Glu Ala Thr Asn Pro Ile Gly Thr Arg Ser Gly Gln Val 320 325 330 Glu Val Asn Ile Thr Glu Phe Pro Tyr Thr Pro Ser Pro Pro Glu 335 340 345 His Gly Arg Arg Ala Gly Pro Val Pro Thr Ala Ile Ile Gly Gly 350 355 360 Val Ala Gly Ser Ile Leu Leu Val Leu Ile Val Val Gly Gly Ile 365 370 375 Val Val Ala Leu Arg Arg Arg Arg His Thr Phe Lys Gly Asp Tyr 380 385 390 Ser Thr Lys Lys His Val Tyr Gly Asn Gly Tyr Ser Lys Ala Gly 395 400 405 Ile Pro Gln His His Pro Pro Met Ala Gln Asn Leu Gln Tyr Pro 410 415 420 Asp Asp Ser Asp Asp Glu Lys Lys Ala Gly Pro Leu Gly Gly Ser 425 430 435 Ser Tyr Glu Glu Glu Glu Glu Glu Glu Glu Gly Gly Gly Gly Gly 440 445 450 Glu Arg Lys Val Gly Gly Pro His Pro Lys Tyr Asp Glu Asp Ala 455 460 465 Lys Arg Pro Tyr Phe Thr Val Asp Glu Ala Glu Ala Arg Gln Asp 470 475 480 Gly Tyr Gly Asp Arg Thr Leu Gly Tyr Gln Tyr Asp Pro Glu Gln 485 490 495 Leu Asp Leu Ala Glu Asn Met Val Ser Gln Asn Asp Gly Ser Phe 500 505 510 Ile Ser Lys Lys Glu Trp Tyr Val 515 21 1444 DNA Homo sapiens misc_feature Incyte ID No 1650519CB1 21 ggagaatttg aaagggtgcc ccaaaggaca atctctaaag gggtaagggg gatacctacc 60 ttgtctggta ggggagatgt ttcgttttca tgctttacca gaaaatccac ttccctgccg 120 accttagttt caaagcttat tcttaattag agacaagaaa cctgtttcaa cttgaagaca 180 ccgtatgagg tgaatggaca gccagccacc acaatgaaag aaatcaaacc aggaataacc 240 tatgctgaac ccacgcctca atcgtcccca agtgtttcct gacacgcatc tttgcttaca 300 gtgcatcaca actgaagaat ggggttcaac ttgacgcttg caaaattacc aaataacgag 360 ctgcacggcc aagagagtca caattcaggc aacaggagcg acgggccagg aaagaacacc 420 acccttcaca atgaatttga cacaattgtc ttgccggtgc tttatctcat tatatttgtg 480 gcaagcatct tgctgaatgg tttagcagtg tggatcttct tccacattag gaataaaacc 540 agcttcatat tctatctcaa aaacatagtg gttgcagacc tcataatgac gctgacattt 600 ccatttcgaa tagtccatga tgcaggattt ggaccttggt acttcaagtt tattctctgc 660 agatacactt cagttttgtt ttatgcaaac atgtatactt ccatcgtgtt ccttgggctg 720 ataagcattg atcgctatct gaaggtggtc aagccatttg gggactctcg gatgtacagc 780 ataaccttca cgaaggtttt atctgtttgt gtttgggtga tcatggctgt tttgtctttg 840 ccaaacatca tcctgacaaa tggtcagcca acagaggaca atatccatga ctgctcaaaa 900 cttaaaagtc ctttgggggt caaatggcat acggcagtca cctatgtgaa cagctgcttg 960 tttgtggccg tgctggtgat tctgatcgga tgttacatag ccatatccag gtacatccac 1020 aaatccagca ggcaattcat aagtcagtca agccgaaagc gaaaacataa ccagagcatc 1080 agggttgttg tggctgtgta ttttacctgc tttctaccat atcacttgtg cagaatgcct 1140 tctactttta gtcacttaga caggctttta gatgaatctg cacaaaaaat cctatattac 1200 tgcaaagaaa ttacactttt cttgtctgcg tgtaatgttt gcctggatcc aataatttac 1260 tttttcatgt gtaggtcatt ttcaagatgg ctgttcaaaa aatcaaatat cagacccagg 1320 agtgaaagca tcagatcact gcaaagtgtg agaagatcgg aagttcgcat atattatgat 1380 tacactgatg tgtaggcctt ttattgtttg ttggaatcga tatgtacaaa gtgtaataca 1440 tcag 1444 22 358 PRT Homo sapiens misc_feature Incyte ID No 1650519CD1 22 Met Gly Phe Asn Leu Thr Leu Ala Lys Leu Pro Asn Asn Glu Leu 1 5 10 15 His Gly Gln Glu Ser His Asn Ser Gly Asn Arg Ser Asp Gly Pro 20 25 30 Gly Lys Asn Thr Thr Leu His Asn Glu Phe Asp Thr Ile Val Leu 35 40 45 Pro Val Leu Tyr Leu Ile Ile Phe Val Ala Ser Ile Leu Leu Asn 50 55 60 Gly Leu Ala Val Trp Ile Phe Phe His Ile Arg Asn Lys Thr Ser 65 70 75 Phe Ile Phe Tyr Leu Lys Asn Ile Val Val Ala Asp Leu Ile Met 80 85 90 Thr Leu Thr Phe Pro Phe Arg Ile Val His Asp Ala Gly Phe Gly 95 100 105 Pro Trp Tyr Phe Lys Phe Ile Leu Cys Arg Tyr Thr Ser Val Leu 110 115 120 Phe Tyr Ala Asn Met Tyr Thr Ser Ile Val Phe Leu Gly Leu Ile 125 130 135 Ser Ile Asp Arg Tyr Leu Lys Val Val Lys Pro Phe Gly Asp Ser 140 145 150 Arg Met Tyr Ser Ile Thr Phe Thr Lys Val Leu Ser Val Cys Val 155 160 165 Trp Val Ile Met Ala Val Leu Ser Leu Pro Asn Ile Ile Leu Thr 170 175 180 Asn Gly Gln Pro Thr Glu Asp Asn Ile His Asp Cys Ser Lys Leu 185 190 195 Lys Ser Pro Leu Gly Val Lys Trp His Thr Ala Val Thr Tyr Val 200 205 210 Asn Ser Cys Leu Phe Val Ala Val Leu Val Ile Leu Ile Gly Cys 215 220 225 Tyr Ile Ala Ile Ser Arg Tyr Ile His Lys Ser Ser Arg Gln Phe 230 235 240 Ile Ser Gln Ser Ser Arg Lys Arg Lys His Asn Gln Ser Ile Arg 245 250 255 Val Val Val Ala Val Tyr Phe Thr Cys Phe Leu Pro Tyr His Leu 260 265 270 Cys Arg Met Pro Ser Thr Phe Ser His Leu Asp Arg Leu Leu Asp 275 280 285 Glu Ser Ala Gln Lys Ile Leu Tyr Tyr Cys Lys Glu Ile Thr Leu 290 295 300 Phe Leu Ser Ala Cys Asn Val Cys Leu Asp Pro Ile Ile Tyr Phe 305 310 315 Phe Met Cys Arg Ser Phe Ser Arg Trp Leu Phe Lys Lys Ser Asn 320 325 330 Ile Arg Pro Arg Ser Glu Ser Ile Arg Ser Leu Gln Ser Val Arg 335 340 345 Arg Ser Glu Val Arg Ile Tyr Tyr Asp Tyr Thr Asp Val 350 355 23 5933 DNA Homo sapiens misc_feature Incyte ID No 474630.4 23 caggacgggc gcacagcagc agccgaggct ggccgggaga gggaggaaga ggatggcagg 60 gccacgcccc agcccatggg ccaggctgct cctggcagcc ttgatcagcg tcagcctctc 120 tgggaccttg gcaactgacc actgcccacc ttcagggctg gaaaacttga ggctccaagc 180 tcttcagcct agagaagctt gagccctgac cacggggcct gagaatagga gcgaaggagg 240 ctgtgtctag aggaaagagg agacacccac ccaggactga ggcacccaga ggatgcactg 300 aggccccaga gcaaaccgct gcaagaaggc cccagtgaag agctgcacgg agtgtgtccg 360 tgtggataag gactgcgcct actgcacaga cgagatgttc agggaccggc gctgcaacac 420 ccaggcggag ctgctggccg cgggctgcca gcgggagagc atcgtggtca tggagagcag 480 cttccaaatc acagaggaga cccagattga caccaccctg cggcgcagcc agatgtcccc 540 ccaaggcctg cgggtccgtc tgcggcccgg tgaggagcgg cattttgagc tggaggtgtt 600 tgagccactg gagagccccg tggacctgta catcctcatg gacttctcca actccatgtc 660 cgatgatctg gacaacctca agaagatggg gcagaacctg gctcgggtcc tgagccagct 720 caccagcgac tacactattg gatttggcaa gtttgtggac aaagtcagcg tcccgcagac 780 ggacatgagg cctgagaagc tgaaggagcc ttggcccaac agtgaccccc ccttctcctt 840 caagaacgtc atcagcctga cagaagatgt ggatgagttc cggaataaac tgcagggaga 900 gcggatctca ggcaacctgg atgctcctga gggcggcttc gatgccatcc tgcagacagc 960 tgtgtgcacg agggacattg gctggcgccc ggacagcacc cacctgctgg tcttctccac 1020 cgagtcagcc ttccactatg aggctgatgg cgccaacgtg ctggctggca tcatgagccg 1080 caacgatgaa cggtgccacc tggacaccac gggcacctac acccagtaca ggacacagga 1140 ctacccgtcg gtgcccaccc tggtgcgcct gctcgccaag cacaacatca tccccatctt 1200 tgcttgtcac caactactcc tatagctact acgagaagct tcacacctat ttccctgtct 1260 cctcactggg ggtgctgcag gaggactcgt ccaacatcgt ggagctgctg gaggaggcct 1320 tcaatcggat ccgctccaac ctggacatcc gggccctaga cagcccccga ggccttcgga 1380 cagaggtcac ctccaagatg ttccagaaga cgaggactgg gtcctttcac atccggcggg 1440 gggaagtggg tatataccag gtgcagctgc gggcccttga gcacgtggat gggacgcacg 1500 tgtgccagct gccggaggac cagaagggca acatccatct gaaaccttcc ttctccgacg 1560 gcctcaagat ggacgcgggc atcatctgtg atgtgtgcac ctgcgagctg caaaaagagg 1620 tgcggtcagc tcgctgcagc ttcaacggag acttcgtgtg cggacagtgt gtgtgcagcg 1680 agggctggag tggccagacc tgcaactgct ccaccggctc tctgagtgac attcagccct 1740 gcctgcggga gggcgaggac aagccgtgct ccggccgtgg ggagtgccag tgcgggcact 1800 gtgtgtgcta cggcgaaggc cgctacgagg gtcagttctg cgagtatgac aacttccagt 1860 gtccccgcac ttccgggttc ctgtgcaatg accgaggacg ctgctccatg ggccagtgtg 1920 tgtgtgagcc tggttggaca ggcccaagct gtgactgtcc cctcagcaat gccacctgca 1980 tcgacagcaa tgggggcatc tgtaatggac gtggccactg tgagtgtggc cgctgccact 2040 gccaccagca gtcgctctac acggacacca tctgcgagat caactactcg gcgatccacc 2100 cgggcctctg cgaggaccta cgctcctgcg tgcagtgcca ggcgtggggc accggcgaga 2160 agaaggggcg cacgtgtgag gaatgcaact tcaaggtcaa gatggtggac gagcttaaga 2220 gagccgagga ggtggtggtg cgctgctcct tccgggacga ggatgacgac tgcacctaca 2280 gctacaccat ggaaggtgac ggcgcccctg ggcccaacag cactgtcctg gtgcacaaga 2340 agaaggactg ccctccgggc tccttctggt ggnnnnnnnn nnnnnnnnnn nnnnnnnnnn 2400 nnnnnnnggc cctgctactg ctgctatgct ggaagtactg tgcctgctgc aaggcctgcc 2460 tggcacttct cccgtgctgc aaccgaggtc acatggtggg ctttaaggaa gaccactaca 2520 tgctgcggga gaacctgatg gcctctgacc acttggacac gcccatgctg cgcagcggga 2580 acctcaaggg ccgtgacgtg gtccgctgga aggtcaccaa caacatgcag cggcctggct 2640 ttgccactca tgccgccagc atcaacccca cagagctggt gccctacggg ctgtccttgc 2700 gcctggcccg cctttgcacc gagaacctgc tgaagcctga cactcgggag tgcgcccagc 2760 tgcgccagga ggtggaggag aacctgaacg aggtctacag gcagatctcc ggtgtacaca 2820 agctccagca gaccaagttc cggcagcagc ccaatgccgg gaaaaagcaa gaccacacca 2880 ttgtggacac agtgctgatg gcgccccgct cggccaagcc ggccctgctg aagcttacag 2940 agaagcaggt ggaacagagg gccttccacg acctcaaggt ggcccccggc tactacaccc 3000 tcactgcaga ccaggacgcc cggggcatgg tggagttcca ggagggcgtg gagctggtgg 3060 acgtacgggt gcccctcttt atccggcctg aggatgacga cgagaagcag ctgctggtgg 3120 aggccatcga cgtgcccgca ggcactgcca ccctcggccg ccgcctggta aacatcacca 3180 tcatcaagga gcaagccaga gacgtggtgt cctttgagca gcctgagttc tcggtcagcc 3240 gcggggacca ggtggcccgc atccctgtca tccggcgtgt cctggacggc gggaagtccc 3300 aggtctccta ccgcacacag gatggcaccg cgcagggcaa ccgggactac atccccgtgg 3360 agggtgagct gctgttccag cctggggagg cctggaaaga gctgcaggtg aagctcctgg 3420 agctgcaaga agttgactcc ctcctgcggg gccgccaggt ccgccgtttc cacgtccagc 3480 tcagcaaccc taagtttggg gcccacctgg gccagcccca ctccaccacc atcatcatca 3540 gggacccaga tgaactggac cggagcttca cgagtcagat gttgtcatca cagccacccc 3600 ctcacggcga cctgggcgcc ccgcagaacc ccaatgctaa ggccgctggg tccaggaaga 3660 tccatttcaa ctggctgccc ccttctggca agccaatggg gtacagggta aagtactgga 3720 ttcagggtga ctccgaatcc gaagcccacc tgctcgacag caaggtgccc tcagtggagc 3780 tcaccaacct gtacccgtat tgcgactatg agatgaaggt gtgcgcctac ggggctcagg 3840 gcgagggacc ctacagctcc ctggtgtcct gccgcaccca ccaggaagtg cccagcgagc 3900 cagggcgtct ggccttcaat gtcgtctcct ccacggtgac ccagctgagc tgggctgagc 3960 cggctgagac caacggtgag atcacagcct acgaggtctg ctatggcctg gtcaacgatg 4020 acaaccgacc tattgggccc atgaagaaag tgctggttga caaccctaag aaccggatgc 4080 tgcttattga gaaccttcgg gagtcccagc cctaccgcta cacggtgaag gcgcgcaacg 4140 gggccggctg ggggcctgag cgggaggcca tcatcaacct ggccacccag cccaagaggc 4200 ccatgtccat ccccatcatc cctgacatcc ctatcgtgga cgcccagagc ggggaggact 4260 acgacagctt ccttatgtac agcgatgacg ttctacgctc tccatcgggc agccagaggc 4320 ccagcgtctc cgatgacact gagcacctgg tgaatggccg gatggacttt gccttcccgg 4380 gcagcaccaa ctccctgcac aggatgacca cgaccagtgc tgctgcctat ggcacccacc 4440 tgagcccaca cgtgccccac cgcgtgctaa gcacatcctc caccctcaca cgggactaca 4500 actcactgac ccgctcagaa cactcacact cgaccacact gcccagggac tactccaccc 4560 tcacctccgt ctcctcccac ggcctccctc ccatctggga acacgggagg agcaggcttc 4620 cgctgtcctg ggccctgggg tcccggagtc gggctcagat gaaagggttc cccccttcca 4680 ggggcccacg agactctata atcctggctg ggaggccagc agcgccctcc tggggcccag 4740 actctcgcct gactgctggt gtgcccgaca cgcccacccg cctggtgttc tctgccctgg 4800 ggcccacatc tctcagagtg agctggcagg agccgcggtg cgagcggccg ctgcagggct 4860 acagtgtgga gtaccagctg ctgaacggcg gtgagctgca tcggctcaac atccccaacc 4920 ctgcccagac ctcggtggtg gtggaagacc tcctgcccaa ccactcctac gtgttccgcg 4980 tgcgggccca gagccaggaa ggctggggcc gagagcgtga gggtgtcatc accattgaat 5040 cccaggtgca cccgcagagc ccactgtgtc ccctgccagg ctccgccttc actttgagca 5100 ctcccagtgc cccaggcccg ctggtgttca ctgccctgag cccagactcg ctgcagctga 5160 gctgggagcg gccacggagg cccaatgggg atatcgtcgg ctacctggtg acctgtgaga 5220 tggcccaagg aggagggcca gccaccgcat tccgggtgga tggagacagc cccgagagcc 5280 ggctgaccgt gccgggcctc agcgagaacg tgccctacaa gttcaaggtg caggccagga 5340 ccactgaggg cttcgggcca gagcgcgagg gcatcatcac catagagtcc caggatggag 5400 gacccttccc gcagctgggc agccgtgccg ggctcttcca gcacccgctg caaagcgagt 5460 acagcagcat caccaccacc cacaccagcg ccaccgagcc cttcctagtg gatgggccga 5520 ccctgggggc ccagcacctg gaggcaggcg gctccctcac ccggcatgtg acccaggagt 5580 ttgtgagccg gacactgacc accagcggaa cccttagcac ccacatggac caacagttct 5640 tccaaacttg accgcaccct gccccacccc cgccatgtcc cactaggcgt cctcccgact 5700 cctctcccgg agcctcctca gctactccat ccttgcaccc ctgggggccc agcccacccg 5760 catgcacaga gcaggggcta ggtgtctcct gggaggcatg aagggggcaa ggtccgtcct 5820 ctgtgggccc aaacctattt gtaaccaaag agctgggagc agcacaagga cccagccttt 5880 gttctgcact taataaatgg ttttgctact gctaaaaaaa aaaaaaaagc ggc 5933 24 573 DNA Homo sapiens misc_feature Incyte ID No 093496.1 24 aaaagaaaag gaaaagaaaa gtgtggactt ggatgaaatc ttcaggtcca acatttggga 60 ttctaagttc caaagaccag gttggaatca tttctaagaa ggttctggtg gttacacatt 120 cctggagtcc tctactcccc actccctgcc aagctgggcc tgtggataga tgtgatccct 180 cagcctccca gcttcaaaca cctgccaatg gttgacgtga acaacatggg ctcagtctca 240 gctaggatca cacccaaagc ccagcaccca gtaaggtgca ggagccatcc atttccctga 300 gcagagcaga ttaggctgag gaaagcagca gccatgcctt tgcacaatgc atttctaggg 360 cattcttccc acacataatc tcctctgctc attgtcctgt gaagaaactg tggcctggag 420 aggttgagcc actgtgccaa ggccaccaat gcaggtggta tgtgggtggg tgggggcctg 480 gggtggggag cacggcccag gcagggtctg tgctgaccgc ccttgtgttt ggaacctaga 540 catcccccct tgcctggatc tgagctgacc gaa 573 25 269 DNA Homo sapiens misc_feature Incyte ID No 1231633.4 25 accactgaag atcctggtgt cgccatgggc cgccgccccg cccgttgtta ccggtattgt 60 aagaacaagc cgtacccaaa gtctcgcttc tgccgaggtg tccctgccct ggaggctgcc 120 cgaatttgtg ccaataagta catggtaaaa agttgtggca aagatggctt ccatatccgg 180 gtgcggctcc accccttcca cgtcatccgc atcaacaaga tgttgtcctg tgctggggct 240 gacaggctcc aaacaggcat gcgaggtgc 269 26 1743 DNA Homo sapiens misc_feature Incyte ID No 988891.1 26 ggtattcaac agagaaattt ctcagcctcc tacttctgct tttgaaagct ataaaaacag 60 cgagggagaa actggcagat accaaacctc ttcgaggcac aagggcacaa caggctgctc 120 tgggattctc ttcagccaat cttcattgct caagtgtctg aagcagccat ggcagaagta 180 cctgagctcg ccagtgaaat gatggcttat tacagtggca atgaggatga cttgttcttt 240 gaagctgatg gccctaaaca gatgaagtgc tccttccagg acctggacct ctgccctctg 300 gatggcggca tccagctacg aatctccgac caccactaca gcaagggctt caggcaggcc 360 gcgtcagttg ttgtggccat ggacaagctg aggaagatgc tggttccctg cccacagacc 420 ttccaggaga atgacctgag caccttcttt cccttcatct ttgaagaaga acctatcttc 480 ttcgacacat gggataacga ggcttatgtg cacgatgcac ctgtacgatc actgaactgc 540 acgctccggg actcacagca aaaaagcttg gtgatgtctg gtccatatga actgaaagct 600 ctccacctcc agggacagga tatggagcaa caagtggtgt tctccatgtc ctttgtacaa 660 ggagaagaaa gtaatgacaa aatacctgtg gccttgggcc tcaaggaaaa gaatctgtac 720 ctgtcctgcg tgttgaaaga tgataagccc actctacagc tggagagtgt agatcccaaa 780 aattacccaa agaagaagat ggaaaagcga tttgtcttca acaagataga aatcaataac 840 aagctggaat ttgagtctgc ccagttcccc aactggtaca tcagcacctc tcaagcagaa 900 aacatgcccg tcttcctggg agggaccaaa ggcggccagg atataactga cttcaccatg 960 caatttgtgt cttcctaaag agagctgtac ccagagagtc ctgtgctgaa tgtggactca 1020 atccctaggg ctggcagaaa gggaacagaa aggtttttga gtacggctat agcctggact 1080 ttcctgttgt ctacaccaat gcccaactgc ctgccttagg gtagtgctaa gaggatctcc 1140 tgtccatcag ccaggacagt cagctctctc ctttcagggc caatccccag cccttttgtt 1200 gagccaggcc tctctcacct ctcctactca cttaaagccc gcctgacaga aaccacggcc 1260 acatttggtt ctaagaaacc ctctgtcatt cgctcccaca ttctgatgag caaccgcttc 1320 cctatttatt tatttatttg tttgtttgtt ttattcattg gtctaattta ttcaaagggg 1380 gcaagaagta gcagtgtctg taaaagagcc tagtttttaa tagctatgga atcaattcaa 1440 tttggactgg tgtgctctct ttaaatcaag tcctttaatt aagactgaaa atatataagc 1500 tcagattatt taaatgggaa tatttataaa tgagcaaata tcatactgtt caatggttct 1560 gngcttatat attttcagtc ttaattaaag gactggtgtg ctctctttaa atcaagtcct 1620 ttaattaaga ctgaaaatat ataagctcag attatttaaa tgggaatatt tataaatgag 1680 caaatatcat actgttcaat ggttcttcag tgaagtttat ttcagaaaaa aaaaaaaaag 1740 ggg 1743 27 391 DNA Homo sapiens misc_feature Incyte ID No 988891.15 27 attttgctag agantgttct aaaaccattg cactttactt acaactcctg tccggaaggt 60 gcgaggcaac aagtttttac agccttcaca gaggagtttc tggcagcacc tgtacgatca 120 ctgaactgca cgctccggga ctcacagcaa aaaagcttgg tgatgtctgg tccatatgaa 180 ctgaaagctc tccacctcca gggacaggat atggagcaac aagtggtgtt ctccatgtcc 240 tttgtacaag gagaagaaag taatgacaaa atacctgtgg ccttgggcct tcaaggaaaa 300 gaatctgtac ctgtcctgcg tgttgaaaga tggataaagc ccacttctac agctgggaga 360 gtgttaggat ccccaaaaaa atttacccca a 391 28 7045 DNA Homo sapiens misc_feature Incyte ID No 3774181CB1 28 agtttgctcg gaattcggct cgagcagcac ataaaggaga acacagcgta tttcgagttt 60 ttcaatgatg ccaaagaagc tactgattac ttaaggaatc tanaagatgc cattcagcgg 120 aagtacagct gtgatagatc aagcagcatt cacaagctag aagaccttgt tcaggaatca 180 atggaagaga aagaagaact tctgcagtac aaaagcacta tagcaaacct aatgggaaaa 240 gcaaaaacaa taattcaact gaagccaagg aattctgact gtccactcaa aacttctatt 300 ccgatcaaag ctatctgtga ctacagacaa attgagataa ccatttacaa agacgatgaa 360 tgtgttttgg cgaataactc tcatcgtgct aaatggaagg tcattagtcc tactgggaat 420 gaggctatgg tcccatctgt gtgcttcacc gttcctccac caaacaaaga agcggtggac 480 cttgccaaca gaattgagca acagtatcag aatgtcctga ctctttggca tgagtctcac 540 ataaacatga agagtgtagt atcctggcat tatctcatca atgaaattga tagaattcga 600 gctagcaatg tggcttcaat aaagacaatg ctacctggtg aacatcagca agttctaagt 660 aatctacaat ctcgttttga agattttctg gaagatagcc aggaatccca agtcttttca 720 ggctcagata taacacaact ggaaaaggag gttaatgtat gtaagcagta ttatcaagaa 780 cttcttaaat ctgcagaaag agaggagcaa gaggaatcag tttataatct ctacatctct 840 gaagttcgaa acattagact tcggttagag aactgtgaag atcggctgat tagacagatt 900 cgaactcccc tggaaagaga tgatttgcat gaaagtgtgt tcagaatcac agaacaggag 960 aaactaaaga aagagctgga acgacttaaa gatgatttgg gaacaatcac aaataagtgt 1020 gaggagtttt tcagtcaagc agcagcctct tcatcagtcc ctaccctacg atcagagctt 1080 aatgtggtcc ttcagaacat gaaccaagtc tattctatgt cttccactta catagataag 1140 ttgaaaactg ttaacttggt gttaaaaaac actcaagctg cagaagccct cgtaaaactc 1200 tatgaaacta aactgtgtga agaagaagca gttatagctg acaagaataa tattgagaat 1260 ctaataagta ctttaaagca atggagatct gaagtagatg aaaagagaca ggtattccat 1320 gccttagagg atgagttgca gaaagctaaa gccatcagtg atgaaatgtt taaaacgtat 1380 aaagaacggg accttgattt tgactggcac aaagaaaaag cagatcaatt agttgaaagg 1440 tggcaaaatg ttcatgtgca gattgacaac aggttacggg acttagaggg cattggcaaa 1500 tcactgaagt actacagaga cacttaccat cctttagatg attggatcca gcaggttgaa 1560 actactcaga gaaagattca ggaaaatcag cctgaaaata gtaaaaccct agccacacag 1620 ttgaatcaac agaagatgct ggtgtccgaa atagaaatga aacagagcaa aatggacgag 1680 tgtcaaaaat atgcagaaca gtactcagct acagtgaagg actatgaatt acaaacaatg 1740 acctaccggg ccatggtaga ttcacaacaa aaatctccag tgaaacgccg aagaatgcag 1800 agttcagcag atctcattat tcaagagttc atggacctaa ggactcgata tactgccctg 1860 gtcactctca tgacacaata tattaaattt gctggtgatt cattgaagag gctggaagag 1920 gaggagatta aaaggtgtaa ggagacttct gaacatgggg catattcaga tctgcttcag 1980 cgtcagaagg caacagtgct tgagaatagc aaacttacag gaaagataag tgagttggaa 2040 agaatggtag ctgaactaaa gaaacaaaag tcccgagtag aggaagaact tccgaaggtc 2100 agggaggctg cagaaaatga attgagaaag cagcagagaa atgtagaaga tatctctctg 2160 cagaagataa gggctgaaag tgaagccaag cagtaccgca gggaacttga aaccattgtg 2220 agagagaagg aagccgctga aagagaactg gagcgggtga ggcagctcac catagaggcc 2280 gaggctaaaa gagctgccgt ggaagagaac ctcctgaatt ttcgcaatca gttggaggaa 2340 aacaccttta ccagacgaac actggaagat catcttaaaa gaaaagattt aagtctcaat 2400 gatttggagc aacaaaaaaa taaattaatg gaagaattaa gaagaaagag agacaatgag 2460 gaagaactct tgaagctgat aaagcagatg gaaaaagacc ttgcatttca gaaacaggta 2520 gcagagaaac agttgaaaga aaagcagaaa attgaattgg aagcaagaag aaaaataact 2580 gaaattcagt atacatgtag agaaaatgca ttgccagtgt gtccgatcac acaggctaca 2640 tcatgcaggg cagtaacggg tctccagcaa gaacatgaca agcagaaagc agaagaactc 2700 aaacagcagg tagatgaact aacagctgcc aatagaaagg ctgaacaaga catgagagag 2760 ctgacatatg aacttaatgc cctccagctt gaaaaaacgt catctgagga aaaggctcgt 2820 ttgctaaaag ataaactaga tgaaacaaat aatacactca gatgccttaa gttggagctg 2880 gaaaggaagg atcaggcgga gaaagggtat tctcaacaac tcagagagct tggtaggcaa 2940 ttgaatcaaa ccacaggtaa agctgaagaa gccatgcaag aagctagtga tctcaagaaa 3000 ataaagcgca attatcagtt agaattagaa tctcttaatc atgaaaaagg gaaactacaa 3060 agagaagtag acagaatcac aagggcacat gctgtagctg agaagaatat tcagcattta 3120 aattcacaaa ttcattcttt tcgagatgag aaagaattag aaagactaca aatctgccag 3180 agaaaatcag atcatctaaa agaacaattt gagaaaagcc atgagcagtt gcttcaaaat 3240 atcaaagctg aaaaagaaaa taatgataaa atccaaaggc tcaatgaaga attggagaaa 3300 agtaatgagt gtgcagagat gctaaaacaa aaagtagagg agcttactag gcagaataat 3360 gaaaccaaat taatgatgca gagaattcag gcagaatcag agaatatagt tttagagaaa 3420 caaactatcc agcaaagatg tgaagcactg aaaattcagg cagatggttt taaagatcag 3480 ctacgcagca caaatgaaca cttgcataaa cagacaaaaa cagagcagga ttttcaaaga 3540 aaaattaaat gcctagaaga agacctggcg aaaagtcaaa atttggtaag tgaatttaag 3600 caaaagtgtg accaacagaa cattatcatc cagaatacca agaaagaagt tagaaatctg 3660 aatgcggaac tgaatgcttc caaagaagag aagcgacgcg gggagcagaa agttcagcta 3720 caacaagctc aggtgcaaga gttaaataac aggttgaaaa aagtacaaga cgaattacac 3780 ttaaagacca tagaggagca gatgacccac agaaagatgg ttctgtttca ggaagaatct 3840 ggtaaattca aacaatcagc agaggagttt cggaagaaga tggaaaaatt aatggagtcc 3900 aaagtcatca ctgaaaatga tatttcaggc attaggcttg actttgtgtc tcttcaacaa 3960 gaaaactcta gagcccaaga aaatgctaag ctttgtgaaa caaacattaa agaacttgaa 4020 agacagcttc aacagtatcg tgaacaaatg cagcaagggc agcacatgga agcaaatcat 4080 taccaaaaat gtcagaaact tgaggatgag ctgatagccc agaagcgtga ggttgaaaac 4140 ctgaagcaaa aaatggacca acagatcaaa gagcatgaac atcaattagt tttgctccag 4200 tgtgaaattc aaaaaaagag cacagccaaa gactgtacct tcaaaccaga ttttgagatg 4260 acagtgaagg agtgccagca ctctggagag ctgtcctcta gaaacactgg acaccttcac 4320 ccaacaccca gatcccctct gttgagatgg actcaagaac cacagccatt ggaagagaag 4380 tggcagcatc gggttgttga acagataccc aaagaagtcc aattccagcc accaggggct 4440 ccactcgaga aagagaaaag ccagcagtgt tactctgagt acttttctca gacaagcacc 4500 gagttacaga taacttttga tgagacaaac cccattacaa gactgtctga aattgagaag 4560 ataagagacc aagccctgaa caattctaga ccacctgtta ggtatcaaga taacgcatgt 4620 gaaatggaac tggtgaaggt tttgacaccc ttagagatag ctaagaacaa gcagtatgat 4680 atgcatacag aagtcacaac attaaaacaa gaaaagaacc cagttcccag tgctgaagaa 4740 tggatgcttg aagggtgcag agcatctggt ggactcaaga aaggggattt ccttaagaag 4800 ggcttagaac cagagacctt ccagaacttt gatggtgatc atgcatgttc agtcagggat 4860 gatgaattta aattccaagg gcttaggcac actgtgactg ccaggcagtt ggtggaagct 4920 aagcttctgg acatgagaac aattgagcag ctgcgactcg gtcttaagac tgttgaagaa 4980 gttcagaaaa ctcttaacaa gtttctgacg aaagccacct caattgcagg gctttaccta 5040 gaatctacaa aagaaaagat ttcatttgcc tcagcggccg agagaatcat aatagacaaa 5100 atggtggctt tggcattttt agaagctcag gctgcaacag gttttataat tgatcccatt 5160 tcaggtcaga catattctgt tgaagatgca gttcttaaag gagttgttga ccccgaattc 5220 agaattaggc ttcttgaggc agagaaggca gctgtgggat attcttattc ttctaagaca 5280 ttgtcagtgt ttcaagctat ggaaaataga atgcttgaca gacaaaaagg taaacatatc 5340 ttggaagccc agattgccag tgggggtgtc attgaccctg tgagaggcat tcgtgttcct 5400 ccagaaattg ctctgcagca ggggttgttg aataatgcca tcttacagtt tttacatgag 5460 ccatccagca acacaagagt tttccctaat cccaataaca agcaagctct gtattactca 5520 gaattactgc gaatgtgtgt atttgatgta gagtcccaat gctttctgtt tccatttggg 5580 gagaggaaca tttccaatct caatgtcaag aaaacacata gaatttctgt agtagatact 5640 aaaacaggat cagaattgac cgtgtatgag gctttccaga gaaacctgat tgagaaaagt 5700 atatatcttg aactttcagg gcagcaatat cagtggaagg aagctatgtt ttttgaatcc 5760 tatgggcatt cttctcatat gctgactgat actaaaacag gattacactt caatattaat 5820 gaggctatag agcagggaac aattgacaaa gccttggtca aaaagtatca ggaaggcctc 5880 atcacactta cagaacttgc tgattctttg ctgagccggt tagtccccaa gaaagatttg 5940 cacagtcctg ttgcagggta ttggctgact gctagtgggg aaaggatctc tgtactaaaa 6000 gcctcccgta gaaatttggt tgatcggatt actgccctcc gatgccttga agcccaagtc 6060 agtacagggg gcataattga tcctcttact ggcaaaaagt accgggtggc cgaagctttg 6120 catagaggcc tggttgatga ggggtttgcc cagcagctgc gacagtgtga attagtaatc 6180 acagggattg gccatcccat cactaacaaa atgatgtcag tggtggaagc tgtgaatgca 6240 aatattataa ataaggaaat gggaatccga tgtttggaat ttcagtactt gacaggaggg 6300 ttgatagagc cacaggttca ctctcggtta tcaatagaag aggctctcca agtaggtatt 6360 atagatgtcc tcattgccac aaaactcaaa gatcaaaagt catatgtcag aaatataata 6420 tgccctcaga caaaaagaaa gttgacatat aaagaagcct tagaaaaagc tgattttgat 6480 ttccacacag gacttaaact gttagaagta tctgagcccc tgatgacagg aatttctagc 6540 ctctactatt cttcctaatg ggacatgttt aaataactgt gcaaggggtg atgcaggctg 6600 gttcatgcca ctttttcaga gtatgatgat atcggctaca tatgcagtct gtgaattatg 6660 taacatactc tatttcttga gggctgcaaa ttgctaagtg ctcaaaatag agtaagtttt 6720 aaattgaaaa ttacataaga tttaatgccc ttcaaatggt ttcatttagc cttgagaatg 6780 gttttttgaa acttggccac actaaaatgt tttttttttt ttacgtagaa tgtgggataa 6840 acttgatgaa ctccaagttc acagtgtcat ttcttcagaa ctccccttca ttgaatagtg 6900 atcatttatt aaatgataaa ttgcactcgc tgaaagagca cagtcatgag gcacctggan 6960 atccaagggg aaggtataaa ttccgttcca acggccttca ggtggcgtgt tttgggttgc 7020 ttccaaaatg gaaagttttg ccttt 7045 29 2125 PRT Homo sapiens misc_feature Incyte ID No 3774181CD1 29 Met Glu Glu Lys Glu Glu Leu Leu Gln Tyr Lys Ser Thr Ile Ala 1 5 10 15 Asn Leu Met Gly Lys Ala Lys Thr Ile Ile Gln Leu Lys Pro Arg 20 25 30 Asn Ser Asp Cys Pro Leu Lys Thr Ser Ile Pro Ile Lys Ala Ile 35 40 45 Cys Asp Tyr Arg Gln Ile Glu Ile Thr Ile Tyr Lys Asp Asp Glu 50 55 60 Cys Val Leu Ala Asn Asn Ser His Arg Ala Lys Trp Lys Val Ile 65 70 75 Ser Pro Thr Gly Asn Glu Ala Met Val Pro Ser Val Cys Phe Thr 80 85 90 Val Pro Pro Pro Asn Lys Glu Ala Val Asp Leu Ala Asn Arg Ile 95 100 105 Glu Gln Gln Tyr Gln Asn Val Leu Thr Leu Trp His Glu Ser His 110 115 120 Ile Asn Met Lys Ser Val Val Ser Trp His Tyr Leu Ile Asn Glu 125 130 135 Ile Asp Arg Ile Arg Ala Ser Asn Val Ala Ser Ile Lys Thr Met 140 145 150 Leu Pro Gly Glu His Gln Gln Val Leu Ser Asn Leu Gln Ser Arg 155 160 165 Phe Glu Asp Phe Leu Glu Asp Ser Gln Glu Ser Gln Val Phe Ser 170 175 180 Gly Ser Asp Ile Thr Gln Leu Glu Lys Glu Val Asn Val Cys Lys 185 190 195 Gln Tyr Tyr Gln Glu Leu Leu Lys Ser Ala Glu Arg Glu Glu Gln 200 205 210 Glu Glu Ser Val Tyr Asn Leu Tyr Ile Ser Glu Val Arg Asn Ile 215 220 225 Arg Leu Arg Leu Glu Asn Cys Glu Asp Arg Leu Ile Arg Gln Ile 230 235 240 Arg Thr Pro Leu Glu Arg Asp Asp Leu His Glu Ser Val Phe Arg 245 250 255 Ile Thr Glu Gln Glu Lys Leu Lys Lys Glu Leu Glu Arg Leu Lys 260 265 270 Asp Asp Leu Gly Thr Ile Thr Asn Lys Cys Glu Glu Phe Phe Ser 275 280 285 Gln Ala Ala Ala Ser Ser Ser Val Pro Thr Leu Arg Ser Glu Leu 290 295 300 Asn Val Val Leu Gln Asn Met Asn Gln Val Tyr Ser Met Ser Ser 305 310 315 Thr Tyr Ile Asp Lys Leu Lys Thr Val Asn Leu Val Leu Lys Asn 320 325 330 Thr Gln Ala Ala Glu Ala Leu Val Lys Leu Tyr Glu Thr Lys Leu 335 340 345 Cys Glu Glu Glu Ala Val Ile Ala Asp Lys Asn Asn Ile Glu Asn 350 355 360 Leu Ile Ser Thr Leu Lys Gln Trp Arg Ser Glu Val Asp Glu Lys 365 370 375 Arg Gln Val Phe His Ala Leu Glu Asp Glu Leu Gln Lys Ala Lys 380 385 390 Ala Ile Ser Asp Glu Met Phe Lys Thr Tyr Lys Glu Arg Asp Leu 395 400 405 Asp Phe Asp Trp His Lys Glu Lys Ala Asp Gln Leu Val Glu Arg 410 415 420 Trp Gln Asn Val His Val Gln Ile Asp Asn Arg Leu Arg Asp Leu 425 430 435 Glu Gly Ile Gly Lys Ser Leu Lys Tyr Tyr Arg Asp Thr Tyr His 440 445 450 Pro Leu Asp Asp Trp Ile Gln Gln Val Glu Thr Thr Gln Arg Lys 455 460 465 Ile Gln Glu Asn Gln Pro Glu Asn Ser Lys Thr Leu Ala Thr Gln 470 475 480 Leu Asn Gln Gln Lys Met Leu Val Ser Glu Ile Glu Met Lys Gln 485 490 495 Ser Lys Met Asp Glu Cys Gln Lys Tyr Ala Glu Gln Tyr Ser Ala 500 505 510 Thr Val Lys Asp Tyr Glu Leu Gln Thr Met Thr Tyr Arg Ala Met 515 520 525 Val Asp Ser Gln Gln Lys Ser Pro Val Lys Arg Arg Arg Met Gln 530 535 540 Ser Ser Ala Asp Leu Ile Ile Gln Glu Phe Met Asp Leu Arg Thr 545 550 555 Arg Tyr Thr Ala Leu Val Thr Leu Met Thr Gln Tyr Ile Lys Phe 560 565 570 Ala Gly Asp Ser Leu Lys Arg Leu Glu Glu Glu Glu Ile Lys Arg 575 580 585 Cys Lys Glu Thr Ser Glu His Gly Ala Tyr Ser Asp Leu Leu Gln 590 595 600 Arg Gln Lys Ala Thr Val Leu Glu Asn Ser Lys Leu Thr Gly Lys 605 610 615 Ile Ser Glu Leu Glu Arg Met Val Ala Glu Leu Lys Lys Gln Lys 620 625 630 Ser Arg Val Glu Glu Glu Leu Pro Lys Val Arg Glu Ala Ala Glu 635 640 645 Asn Glu Leu Arg Lys Gln Gln Arg Asn Val Glu Asp Ile Ser Leu 650 655 660 Gln Lys Ile Arg Ala Glu Ser Glu Ala Lys Gln Tyr Arg Arg Glu 665 670 675 Leu Glu Thr Ile Val Arg Glu Lys Glu Ala Ala Glu Arg Glu Leu 680 685 690 Glu Arg Val Arg Gln Leu Thr Ile Glu Ala Glu Ala Lys Arg Ala 695 700 705 Ala Val Glu Glu Asn Leu Leu Asn Phe Arg Asn Gln Leu Glu Glu 710 715 720 Asn Thr Phe Thr Arg Arg Thr Leu Glu Asp His Leu Lys Arg Lys 725 730 735 Asp Leu Ser Leu Asn Asp Leu Glu Gln Gln Lys Asn Lys Leu Met 740 745 750 Glu Glu Leu Arg Arg Lys Arg Asp Asn Glu Glu Glu Leu Leu Lys 755 760 765 Leu Ile Lys Gln Met Glu Lys Asp Leu Ala Phe Gln Lys Gln Val 770 775 780 Ala Glu Lys Gln Leu Lys Glu Lys Gln Lys Ile Glu Leu Glu Ala 785 790 795 Arg Arg Lys Ile Thr Glu Ile Gln Tyr Thr Cys Arg Glu Asn Ala 800 805 810 Leu Pro Val Cys Pro Ile Thr Gln Ala Thr Ser Cys Arg Ala Val 815 820 825 Thr Gly Leu Gln Gln Glu His Asp Lys Gln Lys Ala Glu Glu Leu 830 835 840 Lys Gln Gln Val Asp Glu Leu Thr Ala Ala Asn Arg Lys Ala Glu 845 850 855 Gln Asp Met Arg Glu Leu Thr Tyr Glu Leu Asn Ala Leu Gln Leu 860 865 870 Glu Lys Thr Ser Ser Glu Glu Lys Ala Arg Leu Leu Lys Asp Lys 875 880 885 Leu Asp Glu Thr Asn Asn Thr Leu Arg Cys Leu Lys Leu Glu Leu 890 895 900 Glu Arg Lys Asp Gln Ala Glu Lys Gly Tyr Ser Gln Gln Leu Arg 905 910 915 Glu Leu Gly Arg Gln Leu Asn Gln Thr Thr Gly Lys Ala Glu Glu 920 925 930 Ala Met Gln Glu Ala Ser Asp Leu Lys Lys Ile Lys Arg Asn Tyr 935 940 945 Gln Leu Glu Leu Glu Ser Leu Asn His Glu Lys Gly Lys Leu Gln 950 955 960 Arg Glu Val Asp Arg Ile Thr Arg Ala His Ala Val Ala Glu Lys 965 970 975 Asn Ile Gln His Leu Asn Ser Gln Ile His Ser Phe Arg Asp Glu 980 985 990 Lys Glu Leu Glu Arg Leu Gln Ile Cys Gln Arg Lys Ser Asp His 995 1000 1005 Leu Lys Glu Gln Phe Glu Lys Ser His Glu Gln Leu Leu Gln Asn 1010 1015 1020 Ile Lys Ala Glu Lys Glu Asn Asn Asp Lys Ile Gln Arg Leu Asn 1025 1030 1035 Glu Glu Leu Glu Lys Ser Asn Glu Cys Ala Glu Met Leu Lys Gln 1040 1045 1050 Lys Val Glu Glu Leu Thr Arg Gln Asn Asn Glu Thr Lys Leu Met 1055 1060 1065 Met Gln Arg Ile Gln Ala Glu Ser Glu Asn Ile Val Leu Glu Lys 1070 1075 1080 Gln Thr Ile Gln Gln Arg Cys Glu Ala Leu Lys Ile Gln Ala Asp 1085 1090 1095 Gly Phe Lys Asp Gln Leu Arg Ser Thr Asn Glu His Leu His Lys 1100 1105 1110 Gln Thr Lys Thr Glu Gln Asp Phe Gln Arg Lys Ile Lys Cys Leu 1115 1120 1125 Glu Glu Asp Leu Ala Lys Ser Gln Asn Leu Val Ser Glu Phe Lys 1130 1135 1140 Gln Lys Cys Asp Gln Gln Asn Ile Ile Ile Gln Asn Thr Lys Lys 1145 1150 1155 Glu Val Arg Asn Leu Asn Ala Glu Leu Asn Ala Ser Lys Glu Glu 1160 1165 1170 Lys Arg Arg Gly Glu Gln Lys Val Gln Leu Gln Gln Ala Gln Val 1175 1180 1185 Gln Glu Leu Asn Asn Arg Leu Lys Lys Val Gln Asp Glu Leu His 1190 1195 1200 Leu Lys Thr Ile Glu Glu Gln Met Thr His Arg Lys Met Val Leu 1205 1210 1215 Phe Gln Glu Glu Ser Gly Lys Phe Lys Gln Ser Ala Glu Glu Phe 1220 1225 1230 Arg Lys Lys Met Glu Lys Leu Met Glu Ser Lys Val Ile Thr Glu 1235 1240 1245 Asn Asp Ile Ser Gly Ile Arg Leu Asp Phe Val Ser Leu Gln Gln 1250 1255 1260 Glu Asn Ser Arg Ala Gln Glu Asn Ala Lys Leu Cys Glu Thr Asn 1265 1270 1275 Ile Lys Glu Leu Glu Arg Gln Leu Gln Gln Tyr Arg Glu Gln Met 1280 1285 1290 Gln Gln Gly Gln His Met Glu Ala Asn His Tyr Gln Lys Cys Gln 1295 1300 1305 Lys Leu Glu Asp Glu Leu Ile Ala Gln Lys Arg Glu Val Glu Asn 1310 1315 1320 Leu Lys Gln Lys Met Asp Gln Gln Ile Lys Glu His Glu His Gln 1325 1330 1335 Leu Val Leu Leu Gln Cys Glu Ile Gln Lys Lys Ser Thr Ala Lys 1340 1345 1350 Asp Cys Thr Phe Lys Pro Asp Phe Glu Met Thr Val Lys Glu Cys 1355 1360 1365 Gln His Ser Gly Glu Leu Ser Ser Arg Asn Thr Gly His Leu His 1370 1375 1380 Pro Thr Pro Arg Ser Pro Leu Leu Arg Trp Thr Gln Glu Pro Gln 1385 1390 1395 Pro Leu Glu Glu Lys Trp Gln His Arg Val Val Glu Gln Ile Pro 1400 1405 1410 Lys Glu Val Gln Phe Gln Pro Pro Gly Ala Pro Leu Glu Lys Glu 1415 1420 1425 Lys Ser Gln Gln Cys Tyr Ser Glu Tyr Phe Ser Gln Thr Ser Thr 1430 1435 1440 Glu Leu Gln Ile Thr Phe Asp Glu Thr Asn Pro Ile Thr Arg Leu 1445 1450 1455 Ser Glu Ile Glu Lys Ile Arg Asp Gln Ala Leu Asn Asn Ser Arg 1460 1465 1470 Pro Pro Val Arg Tyr Gln Asp Asn Ala Cys Glu Met Glu Leu Val 1475 1480 1485 Lys Val Leu Thr Pro Leu Glu Ile Ala Lys Asn Lys Gln Tyr Asp 1490 1495 1500 Met His Thr Glu Val Thr Thr Leu Lys Gln Glu Lys Asn Pro Val 1505 1510 1515 Pro Ser Ala Glu Glu Trp Met Leu Glu Gly Cys Arg Ala Ser Gly 1520 1525 1530 Gly Leu Lys Lys Gly Asp Phe Leu Lys Lys Gly Leu Glu Pro Glu 1535 1540 1545 Thr Phe Gln Asn Phe Asp Gly Asp His Ala Cys Ser Val Arg Asp 1550 1555 1560 Asp Glu Phe Lys Phe Gln Gly Leu Arg His Thr Val Thr Ala Arg 1565 1570 1575 Gln Leu Val Glu Ala Lys Leu Leu Asp Met Arg Thr Ile Glu Gln 1580 1585 1590 Leu Arg Leu Gly Leu Lys Thr Val Glu Glu Val Gln Lys Thr Leu 1595 1600 1605 Asn Lys Phe Leu Thr Lys Ala Thr Ser Ile Ala Gly Leu Tyr Leu 1610 1615 1620 Glu Ser Thr Lys Glu Lys Ile Ser Phe Ala Ser Ala Ala Glu Arg 1625 1630 1635 Ile Ile Ile Asp Lys Met Val Ala Leu Ala Phe Leu Glu Ala Gln 1640 1645 1650 Ala Ala Thr Gly Phe Ile Ile Asp Pro Ile Ser Gly Gln Thr Tyr 1655 1660 1665 Ser Val Glu Asp Ala Val Leu Lys Gly Val Val Asp Pro Glu Phe 1670 1675 1680 Arg Ile Arg Leu Leu Glu Ala Glu Lys Ala Ala Val Gly Tyr Ser 1685 1690 1695 Tyr Ser Ser Lys Thr Leu Ser Val Phe Gln Ala Met Glu Asn Arg 1700 1705 1710 Met Leu Asp Arg Gln Lys Gly Lys His Ile Leu Glu Ala Gln Ile 1715 1720 1725 Ala Ser Gly Gly Val Ile Asp Pro Val Arg Gly Ile Arg Val Pro 1730 1735 1740 Pro Glu Ile Ala Leu Gln Gln Gly Leu Leu Asn Asn Ala Ile Leu 1745 1750 1755 Gln Phe Leu His Glu Pro Ser Ser Asn Thr Arg Val Phe Pro Asn 1760 1765 1770 Pro Asn Asn Lys Gln Ala Leu Tyr Tyr Ser Glu Leu Leu Arg Met 1775 1780 1785 Cys Val Phe Asp Val Glu Ser Gln Cys Phe Leu Phe Pro Phe Gly 1790 1795 1800 Glu Arg Asn Ile Ser Asn Leu Asn Val Lys Lys Thr His Arg Ile 1805 1810 1815 Ser Val Val Asp Thr Lys Thr Gly Ser Glu Leu Thr Val Tyr Glu 1820 1825 1830 Ala Phe Gln Arg Asn Leu Ile Glu Lys Ser Ile Tyr Leu Glu Leu 1835 1840 1845 Ser Gly Gln Gln Tyr Gln Trp Lys Glu Ala Met Phe Phe Glu Ser 1850 1855 1860 Tyr Gly His Ser Ser His Met Leu Thr Asp Thr Lys Thr Gly Leu 1865 1870 1875 His Phe Asn Ile Asn Glu Ala Ile Glu Gln Gly Thr Ile Asp Lys 1880 1885 1890 Ala Leu Val Lys Lys Tyr Gln Glu Gly Leu Ile Thr Leu Thr Glu 1895 1900 1905 Leu Ala Asp Ser Leu Leu Ser Arg Leu Val Pro Lys Lys Asp Leu 1910 1915 1920 His Ser Pro Val Ala Gly Tyr Trp Leu Thr Ala Ser Gly Glu Arg 1925 1930 1935 Ile Ser Val Leu Lys Ala Ser Arg Arg Asn Leu Val Asp Arg Ile 1940 1945 1950 Thr Ala Leu Arg Cys Leu Glu Ala Gln Val Ser Thr Gly Gly Ile 1955 1960 1965 Ile Asp Pro Leu Thr Gly Lys Lys Tyr Arg Val Ala Glu Ala Leu 1970 1975 1980 His Arg Gly Leu Val Asp Glu Gly Phe Ala Gln Gln Leu Arg Gln 1985 1990 1995 Cys Glu Leu Val Ile Thr Gly Ile Gly His Pro Ile Thr Asn Lys 2000 2005 2010 Met Met Ser Val Val Glu Ala Val Asn Ala Asn Ile Ile Asn Lys 2015 2020 2025 Glu Met Gly Ile Arg Cys Leu Glu Phe Gln Tyr Leu Thr Gly Gly 2030 2035 2040 Leu Ile Glu Pro Gln Val His Ser Arg Leu Ser Ile Glu Glu Ala 2045 2050 2055 Leu Gln Val Gly Ile Ile Asp Val Leu Ile Ala Thr Lys Leu Lys 2060 2065 2070 Asp Gln Lys Ser Tyr Val Arg Asn Ile Ile Cys Pro Gln Thr Lys 2075 2080 2085 Arg Lys Leu Thr Tyr Lys Glu Ala Leu Glu Lys Ala Asp Phe Asp 2090 2095 2100 Phe His Thr Gly Leu Lys Leu Leu Glu Val Ser Glu Pro Leu Met 2105 2110 2115 Thr Gly Ile Ser Ser Leu Tyr Tyr Ser Ser 2120 2125 30 1708 DNA Homo sapiens misc_feature Incyte ID No 1709387CB1 30 cctgccagca tctcttgggt ttgctgagaa ctcacgggct ccagctacct ggccatgacc 60 accacatttc tgcaaacttc ttcctccacc tttgggggtg gctcaacccg agggggttcc 120 ctcctggctg ggggaggtgg ctttggtggg gggagtctct ctgggggagg tggaagccga 180 agtatctcag cttcttctgc taggtttgtc tcttcagggt caggaggagg atatgggggt 240 ggcatgaggg tctgtggctt tggtggaggg gctggtagtg ttttcggtgg aggctttgga 300 gggggcgttg gtgggggttt tggtggtggc tttggtggtg gcgatggtgg tctcctctct 360 ggcaatgaga aaattaccat gcagaacctc aatgaccgcc tggcctccta cctggacaag 420 gtacgtgccc tggaggaggc caatgctgac ctggaggtga agatccatga ctggtaccag 480 aagcagaccc cagccagccc agaatgcgac tacagccaat acttcaagac cattgaagag 540 ctccgggaca agatcatggc caccaccatc gacaactccc gggtcatcct ggagatcgac 600 aatgccaggc tggctgcgga cgacttcagg ctcaagtatg agaatgagct ggccctgcgc 660 cagggcgttg aggctgacat caacggcttg cgccgagtcc tggatgagct gaccctggcc 720 aggactgacc tggagatgca gatcgagggc ctgaatgagg agctagccta cctgaagaag 780 aaccacgaag aggagatgaa ggagttcagc agccagctgg ccggccaggt caatgtggag 840 atggacgcag caccgggtgt ggacctgacc cgtgtgctgg cagagatgag ggagcagtac 900 gaggccatgg cggagaagaa ccgccgggat gtcgaggcct ggttcttcag caagactgag 960 gagctgaaca aagaggtggc ctccaacaca gaaatgatcc agaccagcaa gacggagatc 1020 acagacctga gacgcacgat gcaggagctg gagatcgagc tgcagtccca gctcagcatg 1080 aaagctgggc tggagaactc actggccgag acagagtgcc gctatgccac gcagctgcag 1140 cagatccagg ggctcattgg tggcctggag gcccagctga gtgagctccg atgcgagatg 1200 gaggctcaga accaggagta caagatgctg cttgacataa agacacggct ggagcaggag 1260 atcgctactt accgcagcct gctcgagggc caggatgcca agatggctgg cattggcatc 1320 agggaagcct cttcaggagg tggtggtagc agcagcaatt tccacatcaa tgtagaagag 1380 tcagtggatg gacaggtggt ttcttcccac aagagagaaa tctaagtgtc tattgcagga 1440 gaaacgtccc ttgccactcc ccactctcat caggccaagt ggaggactgg ccagagggcc 1500 tgcacatgca aactccagtc cctgccttca gagagctgaa aagggtccct cggtctttta 1560 tttcagggct ttgcatgcgc tctattcccc ctctgcctct ccccaccttc tttggagcaa 1620 ggagatgcag ctgtattgtg taacaagctc atttgtacag tgtctgttca tgtaataaag 1680 aattactttt ccttttgcaa aaaaaaaa 1708 31 456 PRT Homo sapiens misc_feature Incyte ID No 1709387CD1 31 Met Thr Thr Thr Phe Leu Gln Thr Ser Ser Ser Thr Phe Gly Gly 1 5 10 15 Gly Ser Thr Arg Gly Gly Ser Leu Leu Ala Gly Gly Gly Gly Phe 20 25 30 Gly Gly Gly Ser Leu Ser Gly Gly Gly Gly Ser Arg Ser Ile Ser 35 40 45 Ala Ser Ser Ala Arg Phe Val Ser Ser Gly Ser Gly Gly Gly Tyr 50 55 60 Gly Gly Gly Met Arg Val Cys Gly Phe Gly Gly Gly Ala Gly Ser 65 70 75 Val Phe Gly Gly Gly Phe Gly Gly Gly Val Gly Gly Gly Phe Gly 80 85 90 Gly Gly Phe Gly Gly Gly Asp Gly Gly Leu Leu Ser Gly Asn Glu 95 100 105 Lys Ile Thr Met Gln Asn Leu Asn Asp Arg Leu Ala Ser Tyr Leu 110 115 120 Asp Lys Val Arg Ala Leu Glu Glu Ala Asn Ala Asp Leu Glu Val 125 130 135 Lys Ile His Asp Trp Tyr Gln Lys Gln Thr Pro Ala Ser Pro Glu 140 145 150 Cys Asp Tyr Ser Gln Tyr Phe Lys Thr Ile Glu Glu Leu Arg Asp 155 160 165 Lys Ile Met Ala Thr Thr Ile Asp Asn Ser Arg Val Ile Leu Glu 170 175 180 Ile Asp Asn Ala Arg Leu Ala Ala Asp Asp Phe Arg Leu Lys Tyr 185 190 195 Glu Asn Glu Leu Ala Leu Arg Gln Gly Val Glu Ala Asp Ile Asn 200 205 210 Gly Leu Arg Arg Val Leu Asp Glu Leu Thr Leu Ala Arg Thr Asp 215 220 225 Leu Glu Met Gln Ile Glu Gly Leu Asn Glu Glu Leu Ala Tyr Leu 230 235 240 Lys Lys Asn His Glu Glu Glu Met Lys Glu Phe Ser Ser Gln Leu 245 250 255 Ala Gly Gln Val Asn Val Glu Met Asp Ala Ala Pro Gly Val Asp 260 265 270 Leu Thr Arg Val Leu Ala Glu Met Arg Glu Gln Tyr Glu Ala Met 275 280 285 Ala Glu Lys Asn Arg Arg Asp Val Glu Ala Trp Phe Phe Ser Lys 290 295 300 Thr Glu Glu Leu Asn Lys Glu Val Ala Ser Asn Thr Glu Met Ile 305 310 315 Gln Thr Ser Lys Thr Glu Ile Thr Asp Leu Arg Arg Thr Met Gln 320 325 330 Glu Leu Glu Ile Glu Leu Gln Ser Gln Leu Ser Met Lys Ala Gly 335 340 345 Leu Glu Asn Ser Leu Ala Glu Thr Glu Cys Arg Tyr Ala Thr Gln 350 355 360 Leu Gln Gln Ile Gln Gly Leu Ile Gly Gly Leu Glu Ala Gln Leu 365 370 375 Ser Glu Leu Arg Cys Glu Met Glu Ala Gln Asn Gln Glu Tyr Lys 380 385 390 Met Leu Leu Asp Ile Lys Thr Arg Leu Glu Gln Glu Ile Ala Thr 395 400 405 Tyr Arg Ser Leu Leu Glu Gly Gln Asp Ala Lys Met Ala Gly Ile 410 415 420 Gly Ile Arg Glu Ala Ser Ser Gly Gly Gly Gly Ser Ser Ser Asn 425 430 435 Phe His Ile Asn Val Glu Glu Ser Val Asp Gly Gln Val Val Ser 440 445 450 Ser His Lys Arg Glu Ile 455 32 1393 DNA Homo sapiens misc_feature Incyte ID No 1709118CB1 32 ggacagggct ggagatcgag ttcccagttc gtgaaaagga aaaccccctg aagctgtgcc 60 aagatgtgtg acgacgagga gaccaccgcc ctggtgtgcg acaacggctc tgggctggtg 120 aaggccggct ttgcgggcga tgacgcgccc cgcgctgtct tcccgtccat cgtgggccgc 180 ccgcggcacc agggagttat ggtgggtatg ggtcagaagg actcctacgt aggtgatgaa 240 gcccagagca agagaggcat cctgaccctg aagtatccca tcgagcatgg tatcatcacc 300 aactgggacg acatggagaa gatctggcac cacaccttct acaatgagct ccgtgtggct 360 cccgaggagc accccaccct gctcacagag gccccgctga accccaaggc caaccgggag 420 aagatgactc agatcatgtt tgagaccttc aatgtccctg ccatgtacgt ggccatccag 480 gcagtgctat ccctgtatgc ttctggccgt accacaggca ttgttctgga ctctggggat 540 ggtgtaactc acaatgtccc catctatgag ggctacgctt tgccccatgc catcatgcgt 600 ctggttctgg ctggtcggga cctcactgac tacctcatga agatcctcac tgagcgtggc 660 tactcctttg tcaccactgc tgaacgtgaa attgtccgtg acattaaaga gaagctgtgc 720 tatgtcgccc tggattttga gaatgagatg gccacagctg cctcttcctc ctccctggag 780 aagagctatg aactgcctga tggccaagtc atcactattg gcaatgagcg cttccgctgt 840 cctgagacac tcttccagcc ctccttcatt ggtatggaat ctgctggcat ccatgaaaca 900 acttacaata gcatcatgaa gtgtgacatt gatatccgca aggacctgta tgccaacaat 960 gtcttatctg gaggcaccac tatgtaccct ggtattgctg atcgtatgca gaaggaaatc 1020 actgctctgg ctcctagcac catgaagatt aagattattg ctccccctga gcgtaaatac 1080 tctgtctgga ttgggggctc catcctggcc tctctgtcca ccttccagca aatgtggatt 1140 agcaagcaag agtacgatga ggcaggccca tccattgtcc accgcaaatg cttctaagat 1200 gccttctctc tccatctacc ttccagtcag gatgacggta ttatgcttct tggagtcttc 1260 caaaccacct tccctcatct ttcatcaatc attgtacagt ttgtttacac acgtgcaatt 1320 tgtttgtgct tctaatattt attgctttat aaataaacca gaccaggact tgcaacctaa 1380 aaaaaaaaaa aaa 1393 33 377 PRT Homo sapiens misc_feature Incyte ID No 1709118CD1 33 Met Cys Asp Asp Glu Glu Thr Thr Ala Leu Val Cys Asp Asn Gly 1 5 10 15 Ser Gly Leu Val Lys Ala Gly Phe Ala Gly Asp Asp Ala Pro Arg 20 25 30 Ala Val Phe Pro Ser Ile Val Gly Arg Pro Arg His Gln Gly Val 35 40 45 Met Val Gly Met Gly Gln Lys Asp Ser Tyr Val Gly Asp Glu Ala 50 55 60 Gln Ser Lys Arg Gly Ile Leu Thr Leu Lys Tyr Pro Ile Glu His 65 70 75 Gly Ile Ile Thr Asn Trp Asp Asp Met Glu Lys Ile Trp His His 80 85 90 Thr Phe Tyr Asn Glu Leu Arg Val Ala Pro Glu Glu His Pro Thr 95 100 105 Leu Leu Thr Glu Ala Pro Leu Asn Pro Lys Ala Asn Arg Glu Lys 110 115 120 Met Thr Gln Ile Met Phe Glu Thr Phe Asn Val Pro Ala Met Tyr 125 130 135 Val Ala Ile Gln Ala Val Leu Ser Leu Tyr Ala Ser Gly Arg Thr 140 145 150 Thr Gly Ile Val Leu Asp Ser Gly Asp Gly Val Thr His Asn Val 155 160 165 Pro Ile Tyr Glu Gly Tyr Ala Leu Pro His Ala Ile Met Arg Leu 170 175 180 Val Leu Ala Gly Arg Asp Leu Thr Asp Tyr Leu Met Lys Ile Leu 185 190 195 Thr Glu Arg Gly Tyr Ser Phe Val Thr Thr Ala Glu Arg Glu Ile 200 205 210 Val Arg Asp Ile Lys Glu Lys Leu Cys Tyr Val Ala Leu Asp Phe 215 220 225 Glu Asn Glu Met Ala Thr Ala Ala Ser Ser Ser Ser Leu Glu Lys 230 235 240 Ser Tyr Glu Leu Pro Asp Gly Gln Val Ile Thr Ile Gly Asn Glu 245 250 255 Arg Phe Arg Cys Pro Glu Thr Leu Phe Gln Pro Ser Phe Ile Gly 260 265 270 Met Glu Ser Ala Gly Ile His Glu Thr Thr Tyr Asn Ser Ile Met 275 280 285 Lys Cys Asp Ile Asp Ile Arg Lys Asp Leu Tyr Ala Asn Asn Val 290 295 300 Leu Ser Gly Gly Thr Thr Met Tyr Pro Gly Ile Ala Asp Arg Met 305 310 315 Gln Lys Glu Ile Thr Ala Leu Ala Pro Ser Thr Met Lys Ile Lys 320 325 330 Ile Ile Ala Pro Pro Glu Arg Lys Tyr Ser Val Trp Ile Gly Gly 335 340 345 Ser Ile Leu Ala Ser Leu Ser Thr Phe Gln Gln Met Trp Ile Ser 350 355 360 Lys Gln Glu Tyr Asp Glu Ala Gly Pro Ser Ile Val His Arg Lys 365 370 375 Cys Phe 34 2310 DNA Homo sapiens misc_feature Incyte ID No 008513.49 34 cttccctctc tcctccagcc tctcacactc tcctcagctc tctcatctcc tggaaccatg 60 gccagcacat ccaccaccat caggagccac agcagcagcc gccggggttt cagtgccaac 120 ttcagccagg ctccctgggg tcagccgctc tggcttcagc agcgtctccg tgtcccgctc 180 caggggcagt ggtggcctgg gtggtgcatg tggaggagct ggctttggca gccgcagtct 240 gtatggcctg gggggctcca agaggatctc cattggaggg ggcagctgtg ccatcagtgg 300 cggctatggc agcagagccg gaggcagcta tggctttggt ggcgccggga gtggatttgg 360 tttcggtggt ggagccggca ttggctttgg tctgggtggt ggagccggcc ttgctggtgg 420 ctttgggggc cctggcttcc ctgtgtgccc ccctggaggc atccaagagg tcaccgtcaa 480 ccagagtctc ctgactcccc tcaacctgca aatcgatccc accatccagc gggtgcgggc 540 cgaggagcgt gagcagatca agaccctcaa caacaagttt gcctccttca tcgacaaggt 600 gcggttcctg gagcagcaga acaaggttct ggaaacaaag tggaccctgc tgcaggagca 660 gggcaccaag actgtgaggc agaacctgga gccgttgttc gagcagtaca tcaacaacct 720 caggaggcag ctggacagca ttgtcgggga acggggccgc ctggactcag agctcagagg 780 catgcaggac ctggtggagg acttcaagaa caaatatgag gatgaaatca acaagcgcac 840 agcagcagag aatgaatttg tgactctgaa gaaggatgtg gatgctgcct acatgaacaa 900 ggttgaactg caagccaagg cagacactct cacagacgag atcaacttcc tgagagcctt 960 gtatgatgca gagctgtccc agatgcagac ccacatctca gacacatctg tggtgctgtc 1020 catggacaac aaccgcaacc tggacctgga cagcatcatc gctgaggtca aggcccaata 1080 tgaggagatt gctcagagaa gccgggctga ggctgagtcc tggtaccaga ccaagtacga 1140 ggagctgcag gtcacagcag gcagacatgg ggacgacctg cgcaacacca agcaggagat 1200 tgctgagatc aaccgcatga tccagaggct gagatctgag atcgaccacg tcaagaagca 1260 gtgcgccaac ctgcaggccg ccattgctga tgctgagcag cgtggggaga tggccctcaa 1320 ggatgccaag aacaagctgg aagggctgga ggatgccctg cagaaggcca agcaggacct 1380 ggcccggctg ctgaaggagt accaggagct gatgaatgtc aagctggccc tggacgtgga 1440 gatcgccacc taccgcaagc tgctggaggg tgaggagtgc aggctgaatg gcgaaggcgt 1500 tggacaagtc aacatctctg tggtgcagtc caccgtctcc agtggctatg gcggtgccag 1560 tggtgtcggc agtggcttag gcctgggtgg aggaagcagc tactcctatg gcagtggtct 1620 tggcgttgga ggtggcttca gttccagcag tggcagagcc attgggggtg gcctcagctc 1680 tgttggaggc ggcagttcca ccatcaagta caccaccacc tcctcctcca gcaggaagag 1740 ctataagcac taaagtgcgt ctgctagctc tcggtcccac agtcctcagg cccctctctg 1800 gctgcagagc cctctcctca ggttgccttt cctctcctgg cctccagtct cccctgctgt 1860 cccaggtaga gctgggtatg gatgcttagt gccctcactt cttctctctc tctctatacc 1920 atctgagcac ccattgctca ccatcagatc aacctctgat tttacatcat gatgtaatca 1980 ccactggagc ttcactgtta ctaaattatt aatttcttgc ctccagtgtt ctatctctga 2040 ggctgagcat tataagaaaa tgacctctgc tccttttcat tgcagaaaat tgccaggggc 2100 ttatttcaga acaacttcca cttactttcc actggctctc aaactctcta acttataagt 2160 gttgtgaacc cccacccagg cagtatccat gaaagcacaa gtgactagtc ctatgatgta 2220 caaagcctgt atctctgtga tgatttctgt gctcttcgct gtttgcaatt gctaaataaa 2280 gcagatttat aatacaaaaa aaaaaanggg 2310 35 493 DNA Homo sapiens misc_feature Incyte ID No 047568.1 35 cttaacctta attttataag agacaaatac atgttataat aatacttaag ctctttatag 60 aatttgtagg gctattgaga gacattatag ggaagccctt gttctggaag gtgtatggtt 120 gtggccatgg gtttctctgc cactaaatct gtacctggtt gttatttgaa gttttctgtc 180 ctaaaatgta atctttggag aagctgcaca accgccatct gggaactcat gagaaattta 240 cgttttatgc ctaagtaact ctaatgagca atggctatag gaatgactaa taaaatatca 300 acaaggagat gggaattttc aaggaaatat gatatggtaa caatgtcctt tttagaaagt 360 catttttact tatctatatt cacagcataa aatgttccaa aatctatgaa atattaaata 420 ttatacttca aaataaagta atattttgga gataaaagag tactgttcta caattcaaaa 480 ttgaaatagt tca 493 36 1983 DNA Homo sapiens misc_feature Incyte ID No 3120070CB1 36 ggaaccgcct ccccgcggcc tcttcgcttt tgtggcggcg cccgcgctcg caggccactc 60 tctgctgtcg cccgtcccgc gcgctcctcc gacccgctcc gctccgctcc gctcggcccc 120 gcgccgcccg tcaacatgat ccgctgcggc ctggcctgcg agcgctgccg ctggatcctg 180 cccctgctcc tactcagcgc catcgccttc gacatcatcg cgctggccgg ccgcggctgg 240 ttgcagtcta gcgaccacgg ccagacgtcc tcgctgtggt ggaaatgctc ccaagagggc 300 ggcggcagcg ggtcctacga ggagggctgt cagagcctca tggagtacgc gtggggtaga 360 gcagcggctg ccatgctctt ctgtggcttc atcatcctgg tgatctgttt catcctctcc 420 ttcttcgccc tctgtggacc ccagatgctt gtcttcctga gagtgattgg aggtctcctt 480 gccttggctg ctgtgttcca gatcatctcc ctggtaattt accccgtgaa gtacacccag 540 accttcaccc ttcatgccaa ccctgctgtc acttacatct ataactgggc ctacggcttt 600 gggtgggcag ccacgattat cctgattggc tgtgccttct tcttctgctg cctccccaac 660 tacgaagatg accttctggg caatgccaag cccaggtact tctacacatc tgcctaactt 720 gggaatgaat gtgggagaaa atcgctgctg ctgagatgga ctccagaaga agaaactgtt 780 tctccaggcg actttgaacc cattttttgg cagtgttcat attattaaac tagtcaaaaa 840 tgctaaaata atttgggaga aaatattttt taagtagtgt tatagtttca tgtttatctt 900 ttattatgtt ttgtgaagtt gtgtcttttc actaattacc tatactatgc caatatttcc 960 ttatatctat ccataacatt tatactacat ttgtaagaga atatgcacgt gaaacttaac 1020 actttataag gtaaaaatga ggtttccaag atttaataat ctgatcaagt tcttgttatt 1080 tccaaataga atggactcgg tctgttaagg gctaaggaga agaggaagat aaggttaaaa 1140 gttgttaatg accaaacatt ctaaaagaaa tgcaaaaaaa aagtttattt tcaagccttc 1200 gaactattta aggaaagcaa aatcatttcc taaatgcata tcatttgtga gaatttctca 1260 ttaatatcct gaatcattca tttcagctaa ggcttcatgt tgactcgata tgtcatctag 1320 gaaagtacta tttcatggtc caaacctgtt gccatagttg gtaaggcttt cctttaagtg 1380 tgaaatattt agatgaaatt ttctctttta aagttcttta tagggttagg gtgtgggaaa 1440 atgctatatt aataaatctg tagtgttttg tgtttatatg ttcagaacca gagtagactg 1500 gattgaaaga tggactgggt ctaatttatc atgactgata gatctggtta agttgtgtag 1560 taaagcatta gggtcattcc tgtcacaaaa gtgccactaa aacagcctca ggagaataaa 1620 tgacttgctt ttctaaatct caggtttatc tgggctctat catatagaca ggcttctgat 1680 agtttgcaac tgtaagcaga aacctacata tagttaaaat cctggtcttt cttggtaaac 1740 agattttaaa tgtctgatat aaaacatgcc acaggagaat tcggggattt gagtttctct 1800 gaatagcata tatatgatgc atcggatagg tcattatgat tttttaccat ttcgacttac 1860 ataatgaaaa ccaattcatt ttaaatatca gattattatt ttgtaagttg tggaaaaagc 1920 taattgtagt tttcattatg aagttttccc aataaaccag gtattctaaa cttgaaaaaa 1980 aaa 1983 37 193 PRT Homo sapiens misc_feature Incyte ID No 3120070CD1 37 Met Ile Arg Cys Gly Leu Ala Cys Glu Arg Cys Arg Trp Ile Leu 1 5 10 15 Pro Leu Leu Leu Leu Ser Ala Ile Ala Phe Asp Ile Ile Ala Leu 20 25 30 Ala Gly Arg Gly Trp Leu Gln Ser Ser Asp His Gly Gln Thr Ser 35 40 45 Ser Leu Trp Trp Lys Cys Ser Gln Glu Gly Gly Gly Ser Gly Ser 50 55 60 Tyr Glu Glu Gly Cys Gln Ser Leu Met Glu Tyr Ala Trp Gly Arg 65 70 75 Ala Ala Ala Ala Met Leu Phe Cys Gly Phe Ile Ile Leu Val Ile 80 85 90 Cys Phe Ile Leu Ser Phe Phe Ala Leu Cys Gly Pro Gln Met Leu 95 100 105 Val Phe Leu Arg Val Ile Gly Gly Leu Leu Ala Leu Ala Ala Val 110 115 120 Phe Gln Ile Ile Ser Leu Val Ile Tyr Pro Val Lys Tyr Thr Gln 125 130 135 Thr Phe Thr Leu His Ala Asn Pro Ala Val Thr Tyr Ile Tyr Asn 140 145 150 Trp Ala Tyr Gly Phe Gly Trp Ala Ala Thr Ile Ile Leu Ile Gly 155 160 165 Cys Ala Phe Phe Phe Cys Cys Leu Pro Asn Tyr Glu Asp Asp Leu 170 175 180 Leu Gly Asn Ala Lys Pro Arg Tyr Phe Tyr Thr Ser Ala 185 190 38 1516 DNA Homo sapiens misc_feature Incyte ID No 1303785CB1 38 ctttgttttt ggacatagct gagccatgta cttcaaacag aaggcagcca attactaact 60 tctggttgct aggtgtggct tcctttaaaa tcctataaaa tcagaagccc aagtctccac 120 tgccagtgtg aaatcttcag agaagaattt ctctttagtt ctttgcaaga aggtagagat 180 aaagacactt tttcaaaaat ggcaatggta tcagaattcc tcaagcaggc ctggtttatt 240 gaaaatgaag agcaggaata tgttcaaact gtgaagtcat ccaaaggtgg tcccggatca 300 gcggtgagcc cctatcctac cttcaatcca tcctcggatg tcgctgcctt gcataaggcc 360 ataatggtta aaggtgtgga tgaagcaacc atcattgaca ttctaactaa gcgaaacaat 420 gcacagcgtc aacagatcaa agcagcatat ctccaggaaa caggaaagcc cctggatgaa 480 acactgaaga aagcccttac aggtcacctt gaggaggttg ttttagctct gctaaaaact 540 ccagcgcaat ttgatgctga tgaacttcgt gctgccatga agggccttgg aactgatgaa 600 gatactctaa ttgagatttt ggcatcaaga actaacaaag aaatcagaga cattaacagg 660 gtctacagag aggaactgaa gagagatctg gccaaagaca taacctcaga cacatctgga 720 gattttcgga acgctttgct ttctcttgct aagggtgacc gatctgagga ctttggtgtg 780 aatgaagact tggctgattc agatgccagg gccttgtatg aagcaggaga aaggagaaag 840 gggacagacg taaacgtgtt caataccatc cttaccacca gaagctatcc acaacttcgc 900 agagtgtttc agaaatacac caagtacagt aagcatgaca tgaacaaagt tctggacctg 960 gagttgaaag gtgacattga gaaatgcctc acagctatcg tgaagtgcgc cacaagcaaa 1020 ccagctttct ttgcagagaa gcttcatcaa gccatgaaag gtgttggaac tcgccataag 1080 gcattgatca ggattatggt ttcccgttct gaaattgaca tgaatgatat caaagcattc 1140 tatcagaaga tgtatggtat ctccctttgc caagccatcc tggatgaaac caaaggagag 1200 tatgagaaaa tcctggtggc tctttgtgga ggaaactaaa cattcccttg atggtctcaa 1260 gctatgatca gaagacttta attatatatt ttcatcctat aagcttaaat aggaaagttt 1320 cttcaacagg attacagtgt agctacctac atgctgaaaa atatagcctt taaatcattt 1380 ttatattata actctgtata atagagataa gtccattttt taaaaatgtt ttccccaaac 1440 cataaaaccc tatacaagtt gttctagtaa caatacatga gaaagatgtc tatgtagctg 1500 aaaataaaat gncgtc 1516 39 346 PRT Homo sapiens misc_feature Incyte ID No 1303785CD1 39 Met Ala Met Val Ser Glu Phe Leu Lys Gln Ala Trp Phe Ile Glu 1 5 10 15 Asn Glu Glu Gln Glu Tyr Val Gln Thr Val Lys Ser Ser Lys Gly 20 25 30 Gly Pro Gly Ser Ala Val Ser Pro Tyr Pro Thr Phe Asn Pro Ser 35 40 45 Ser Asp Val Ala Ala Leu His Lys Ala Ile Met Val Lys Gly Val 50 55 60 Asp Glu Ala Thr Ile Ile Asp Ile Leu Thr Lys Arg Asn Asn Ala 65 70 75 Gln Arg Gln Gln Ile Lys Ala Ala Tyr Leu Gln Glu Thr Gly Lys 80 85 90 Pro Leu Asp Glu Thr Leu Lys Lys Ala Leu Thr Gly His Leu Glu 95 100 105 Glu Val Val Leu Ala Leu Leu Lys Thr Pro Ala Gln Phe Asp Ala 110 115 120 Asp Glu Leu Arg Ala Ala Met Lys Gly Leu Gly Thr Asp Glu Asp 125 130 135 Thr Leu Ile Glu Ile Leu Ala Ser Arg Thr Asn Lys Glu Ile Arg 140 145 150 Asp Ile Asn Arg Val Tyr Arg Glu Glu Leu Lys Arg Asp Leu Ala 155 160 165 Lys Asp Ile Thr Ser Asp Thr Ser Gly Asp Phe Arg Asn Ala Leu 170 175 180 Leu Ser Leu Ala Lys Gly Asp Arg Ser Glu Asp Phe Gly Val Asn 185 190 195 Glu Asp Leu Ala Asp Ser Asp Ala Arg Ala Leu Tyr Glu Ala Gly 200 205 210 Glu Arg Arg Lys Gly Thr Asp Val Asn Val Phe Asn Thr Ile Leu 215 220 225 Thr Thr Arg Ser Tyr Pro Gln Leu Arg Arg Val Phe Gln Lys Tyr 230 235 240 Thr Lys Tyr Ser Lys His Asp Met Asn Lys Val Leu Asp Leu Glu 245 250 255 Leu Lys Gly Asp Ile Glu Lys Cys Leu Thr Ala Ile Val Lys Cys 260 265 270 Ala Thr Ser Lys Pro Ala Phe Phe Ala Glu Lys Leu His Gln Ala 275 280 285 Met Lys Gly Val Gly Thr Arg His Lys Ala Leu Ile Arg Ile Met 290 295 300 Val Ser Arg Ser Glu Ile Asp Met Asn Asp Ile Lys Ala Phe Tyr 305 310 315 Gln Lys Met Tyr Gly Ile Ser Leu Cys Gln Ala Ile Leu Asp Glu 320 325 330 Thr Lys Gly Glu Tyr Glu Lys Ile Leu Val Ala Leu Cys Gly Gly 335 340 345 Asn 40 2712 DNA Homo sapiens misc_feature Incyte ID No 1798379CB1 40 ccagccttga ctcttctcaa gagcctgtga ctttcctccc tggacaaagg catcatgagt 60 tgtcagatct cttgcaaatc tcgaggaaga ggaggaggtg gaggaggatt ccggggcttc 120 agcagcggct cagctgtggt gtctggtgga agccggagat caacttccag cttctcctgc 180 ttgagccgcc atggtggtgg tggtgggggc ttcggtggag gcggctttgg cagtcggagt 240 cttgttggcc ttggagggac caagagcatc tccattagtg tggctggagg aggtggtggc 300 tttggcgccg ctggtggatt tggtggcaga ggaggtggtt ttggaggcgg cagcggcttt 360 ggaggcggca gcggctttgg aggtggcagc ggcttcagtg gtggtggttt cggtggaggc 420 ggctttggtg gaggccgctt tggaggtttt gggggccctg gtggtgttgg aggtttaggg 480 ggtcctggtg gctttgggcc tggaggatac cctggtggca tccacgaagt ctctgtcaac 540 cagagcctcc tgcagcctct caacgtgaaa gttgacccag agatccagaa tgtgaaggcc 600 caagagcgtg agcagatcaa aactctcaac aacaaatttg cctccttcat tgacaaggtg 660 cggttcttgg agcagcagaa ccaggtgtta cagaccaaat gggagctgct acaacaaatg 720 aatgttggca cccgccccat caacctggag cccatcttcc aggggtatat cgacagcctc 780 aagagatatc tggatgggct cactgcagaa agaacatcac agaattcaga gctgaataac 840 atgcaggatc ttgtggagga ttataagaag aagtatgagg atgaaatcaa taagcgcaca 900 gctgctgaga atgattttgt gacgcttaaa aaggacgtgg acaatgccta catgataaag 960 gtggagttgc agtccaaggt ggacctgctg aaccaggaaa ttgagtttct gaaagttctc 1020 tatgatgcgg agatatccca gatacatcag agtgtcactg acaccaacgt catcctctcc 1080 atggacaaca gccgcaacct ggacttggat agcatcatcg ccgaggtcaa ggcccagtat 1140 gaggagatcg cccagaggag caaggaagaa gcggaggccc tgtaccacag caagtatgag 1200 gagctccagg tgactgtcgg gagacatgga gacagcctga aagagatcaa gatagagatc 1260 agcgagctga accgcgtgat ccagaggctg cagggggaga tcgcacatgt gaagaagcag 1320 tgtaagaatg tgcaagatgc catcgcagat gccgagcagc gtggggagca tgccctcaag 1380 gatgccagga acaagttgaa tgacctggag gaggccctgc agcaggccaa ggaggacttg 1440 gcgcggctgc tgcgtgacta ccaggagctg atgaacgtga agctggccct agatgtggag 1500 atcgccacct accgcaaact gctggagggc gaggagtgca ggatgtctgg agacctcagc 1560 agcaatgtga ctgtgtctgt gacaagcagc accatttcat caaatgtggc atccaaggct 1620 gcctttggag gttctggagg tagagggtcc agttccggag gaggatacag ctctggaagc 1680 agcagttatg gctctggagg ccgacagtct ggctccagag gcggtagtgg aggaggaggt 1740 tctatctctg gaggaggata tggctctggc ggtggttctg gaggaagata cggatctggt 1800 ggtggctcta agggagggtc catctctgga ggaggatatg gctctggagg tggaaaacac 1860 agctctggag gtggctctag aggaggctcc agctctggag gaggatatgg ctctggaggt 1920 gggggttcta gctctgtaaa gggtagctca ggtgaagctt ttggttccag cgtgaccttc 1980 tcttttagat aaagatgagc ccccaccacc accgactctc ccaacccaga ctctcccact 2040 ccagaatgta gaagcctgtc tctgtacctc taactggcag caagttaaat ttttgtcatt 2100 tatctctgat ggcactttga gggaaaagaa tgtccacata cagtttttga aagatcttct 2160 ctccaaacca gttagttaga gccagtgacg cctctgtgtt ctggggcgga atctgtgctg 2220 tctaggtttg tgcttctagc catgcccatt cccgccccca ccatgcctct ttgcattgcc 2280 cattttccag atgtgtattc tgttgaggac ccaggcccat ccagggattt catctctaag 2340 cctggcagtg ctggggggaa atgtgtttct gtgtatatag ctcctcttgt ccactctgct 2400 ttcggaagtg ctgtggtctg ggggtcttca taatataaac ctcatttggc aattcaaaaa 2460 aaaaaaaaag gggggccccc ccacttattt agggggttcc cgacctccaa attcgcgaac 2520 cagggaaaaa ccggtttccc ggtggaaaaa ttgtaacccg cacaaaattt ccccaaaaat 2580 attggccccg gaacctaaaa ggtaaaaact cggggggccc aaagagtttg gcaaacccca 2640 ataatttggg tgggcacaag gcccgtttcc catgggggaa acttttgtgc cacggcttta 2700 ataataggcc cc 2712 41 645 PRT Homo sapiens misc_feature Incyte ID No 1798379CD1 41 Met Ser Cys Gln Ile Ser Cys Lys Ser Arg Gly Arg Gly Gly Gly 1 5 10 15 Gly Gly Gly Phe Arg Gly Phe Ser Ser Gly Ser Ala Val Val Ser 20 25 30 Gly Gly Ser Arg Arg Ser Thr Ser Ser Phe Ser Cys Leu Ser Arg 35 40 45 His Gly Gly Gly Gly Gly Gly Phe Gly Gly Gly Gly Phe Gly Ser 50 55 60 Arg Ser Leu Val Gly Leu Gly Gly Thr Lys Ser Ile Ser Ile Ser 65 70 75 Val Ala Gly Gly Gly Gly Gly Phe Gly Ala Ala Gly Gly Phe Gly 80 85 90 Gly Arg Gly Gly Gly Phe Gly Gly Gly Ser Gly Phe Gly Gly Gly 95 100 105 Ser Gly Phe Gly Gly Gly Ser Gly Phe Ser Gly Gly Gly Phe Gly 110 115 120 Gly Gly Gly Phe Gly Gly Gly Arg Phe Gly Gly Phe Gly Gly Pro 125 130 135 Gly Gly Val Gly Gly Leu Gly Gly Pro Gly Gly Phe Gly Pro Gly 140 145 150 Gly Tyr Pro Gly Gly Ile His Glu Val Ser Val Asn Gln Ser Leu 155 160 165 Leu Gln Pro Leu Asn Val Lys Val Asp Pro Glu Ile Gln Asn Val 170 175 180 Lys Ala Gln Glu Arg Glu Gln Ile Lys Thr Leu Asn Asn Lys Phe 185 190 195 Ala Ser Phe Ile Asp Lys Val Arg Phe Leu Glu Gln Gln Asn Gln 200 205 210 Val Leu Gln Thr Lys Trp Glu Leu Leu Gln Gln Met Asn Val Gly 215 220 225 Thr Arg Pro Ile Asn Leu Glu Pro Ile Phe Gln Gly Tyr Ile Asp 230 235 240 Ser Leu Lys Arg Tyr Leu Asp Gly Leu Thr Ala Glu Arg Thr Ser 245 250 255 Gln Asn Ser Glu Leu Asn Asn Met Gln Asp Leu Val Glu Asp Tyr 260 265 270 Lys Lys Lys Tyr Glu Asp Glu Ile Asn Lys Arg Thr Ala Ala Glu 275 280 285 Asn Asp Phe Val Thr Leu Lys Lys Asp Val Asp Asn Ala Tyr Met 290 295 300 Ile Lys Val Glu Leu Gln Ser Lys Val Asp Leu Leu Asn Gln Glu 305 310 315 Ile Glu Phe Leu Lys Val Leu Tyr Asp Ala Glu Ile Ser Gln Ile 320 325 330 His Gln Ser Val Thr Asp Thr Asn Val Ile Leu Ser Met Asp Asn 335 340 345 Ser Arg Asn Leu Asp Leu Asp Ser Ile Ile Ala Glu Val Lys Ala 350 355 360 Gln Tyr Glu Glu Ile Ala Gln Arg Ser Lys Glu Glu Ala Glu Ala 365 370 375 Leu Tyr His Ser Lys Tyr Glu Glu Leu Gln Val Thr Val Gly Arg 380 385 390 His Gly Asp Ser Leu Lys Glu Ile Lys Ile Glu Ile Ser Glu Leu 395 400 405 Asn Arg Val Ile Gln Arg Leu Gln Gly Glu Ile Ala His Val Lys 410 415 420 Lys Gln Cys Lys Asn Val Gln Asp Ala Ile Ala Asp Ala Glu Gln 425 430 435 Arg Gly Glu His Ala Leu Lys Asp Ala Arg Asn Lys Leu Asn Asp 440 445 450 Leu Glu Glu Ala Leu Gln Gln Ala Lys Glu Asp Leu Ala Arg Leu 455 460 465 Leu Arg Asp Tyr Gln Glu Leu Met Asn Val Lys Leu Ala Leu Asp 470 475 480 Val Glu Ile Ala Thr Tyr Arg Lys Leu Leu Glu Gly Glu Glu Cys 485 490 495 Arg Met Ser Gly Asp Leu Ser Ser Asn Val Thr Val Ser Val Thr 500 505 510 Ser Ser Thr Ile Ser Ser Asn Val Ala Ser Lys Ala Ala Phe Gly 515 520 525 Gly Ser Gly Gly Arg Gly Ser Ser Ser Gly Gly Gly Tyr Ser Ser 530 535 540 Gly Ser Ser Ser Tyr Gly Ser Gly Gly Arg Gln Ser Gly Ser Arg 545 550 555 Gly Gly Ser Gly Gly Gly Gly Ser Ile Ser Gly Gly Gly Tyr Gly 560 565 570 Ser Gly Gly Gly Ser Gly Gly Arg Tyr Gly Ser Gly Gly Gly Ser 575 580 585 Lys Gly Gly Ser Ile Ser Gly Gly Gly Tyr Gly Ser Gly Gly Gly 590 595 600 Lys His Ser Ser Gly Gly Gly Ser Arg Gly Gly Ser Ser Ser Gly 605 610 615 Gly Gly Tyr Gly Ser Gly Gly Gly Gly Ser Ser Ser Val Lys Gly 620 625 630 Ser Ser Gly Glu Ala Phe Gly Ser Ser Val Thr Phe Ser Phe Arg 635 640 645 42 663 DNA Homo sapiens misc_feature Incyte ID No 350650.1 42 ctgggccatg aaaagctccc tggagggaac cctggctgac acagaagctg gctacgtggc 60 tcagctgtca gaaattcaaa cgcagatcag tgccctggag gaggagatct gccagatctg 120 gggtgagact aaatgccaga acgcagagta caagcaattg ctggacatca agacacgcct 180 ggaggtggag atcgagacct accgccgcct gctcgatgga gagggaggtg gttctagttt 240 tgcagaattt ggtggtagaa actccaggat ctgtaaacat ggggatccca gggatctggg 300 tatctggtga ctcaagatct ggaagctgtt ctggtcaagg acgagattca agcaagacta 360 gagtgactaa gactatcgta gaggagttgg tggatggcaa ggttgtctcg tctcaagtca 420 gcagtatttc tgaggtgaaa gttaaataag gaacttccag atcaacaaaa gtgtctttca 480 aagaaaaaaa aatcaagaag gacacaagcg aagaaatggc atcaatctag gcatctttct 540 ggataatttc aggaaaagct tcagtccaga aatggatgac tagccaactt ttctgcatct 600 tcttatttcc tcattagaat gctcttgaaa tagctgaatt aacaactttg ctttaattgt 660 ttg 663 43 809 DNA Homo sapiens misc_feature Incyte ID No 474630.24 43 ccgggagctg gagacgggct cccctcgcag agcctacggc cttcccccgc ctggccctgc 60 tcggcccggc gccccccggc ggtgccaacg cggcccttcg ttgttcccaa tggctgcggc 120 tggaagttcg agcccctgct gggggaggag ctggacctgc ggcgcgtcac gtggcggctg 180 cccccggagc tcatcccgcg cctgtcggcc agcagcgggc gctcctccga cgccgaggcg 240 ccccacgggc ccccggacga cggcggcgcg ggcgggaagg gcggcagcct gccccgcagt 300 gcgacacccg ggccccccgg aggtgacagg ctcacccgcc gccccccgat ccgcgcccac 360 ccagcctcac tcgcgcctga gggccctggg gtgggcgtct gcgctgcctc gggggcccca 420 gtctcagcca ggcacgggcc ttggcggctg ggagcacagc tgctcagagg cagggcccag 480 tgccagggga cgcgtgaggc aggcgcttgg ncccttatgg tgcctgcctg gccagggggt 540 gcaaattcag aagtctgccc gggaagcgga ccctggcacc caagtagacc cctcaggggc 600 ctcaaaggac aggagggaag gcttggggat ctccccaggg cagagctgac tgcagacgca 660 gcaaaccccc gccactgcca gggtcagcag tgctcacacc gatagagtgg ccggccagag 720 gatatgggct gtggaagcct gggtggccct tgggctcctg ctaggacaga gggcctctgt 780 ccctagtggt ttgagggaaa ctggttgta 809 44 295 DNA Homo sapiens misc_feature Incyte ID No 108089.1 44 gggaactagg tcttggccct ttctacagct tttctcctgc aaagggtcca gccttttcct 60 gctccccacg ttgtccttac ggctgtgtgg ggtagggcag ggtccacact ccttcccatc 120 cattttagag gaggaagctg gagtctggga agggatggga ttttcccagg gcaccctgtg 180 agtcacatgc cacttgagac aagggtctag agctccagca ttttccaagc tacaaatgta 240 tctgctgctc caagtgtccg ccagggtcgg cctcagagct ggcaggagtt cggtg 295 45 1744 DNA Homo sapiens misc_feature Incyte ID No 3346307CB1 45 ccaaggggga ggtgcgagcg tggacctggg acgggtctgg gcggctctcg gtggttggca 60 cgggttcgca cacccattca agcggcagga cgcacttgtc ttagcagttc tcgctgaccg 120 cgctagctgc ggcttctacg ctccggcact ctgagttcat cagcaaacgc cctggcgtct 180 gtcctcacca tgcctagcct ttgggaccgc ttctcgtcgt cgtccacctc ctcttcgccc 240 tcgtccttgc cccgaactcc caccccagat cggccgccgc gctcagcctg ggggtcggcg 300 acccgggagg aggggtttga ccgctccacg agcctggaga gctcggactg cgagtccctg 360 gacagcagca acagtggctt cgggccggag gaagacacgg cttacctgga tggggtgtcg 420 ttgcccgact tcgagctgct cagtgaccct gaggatgaac acttgtgtgc caacctgatg 480 cagctgctgc aggagagcct ggcccaggcg cggctgggct ctcgacgccc tgcgcgcctg 540 ctgatgccta gccagttggt aagccaggtg ggcaaagaac tactgcgcct ggcctacagc 600 gagccgtgcg gcctgcgggg ggcgctgctg gacgtctgcg tggagcaggg caagagctgc 660 cacagcgtgg gccagctggc actcgacccc agcctggtgc ccaccttcca gctgaccctc 720 gtgctgcgcc tggactcacg actctggccc aagatccagg ggctgtttag ctccgccaac 780 tctcccttcc tccctggctt cagccagtcc ctgacgctga gcactggctt ccgagtcatc 840 aagaagaagc tgtacagctc ggaacagctg ctcattgagg agtgttgaac ttcaacctga 900 gggggccgac agtgccctcc aagacagaga cgactgaact tttggggtgg agactagagg 960 caggagctga gggactgatt ccagtggttg gaaaactgag gcagccacct aaggtggagg 1020 tgggggaata gtgtttccca ggaagctcat tgagttgtgt gcgggtggct gtgcattggg 1080 gacacatacc cctcagtact gtagcatgaa acaaaggctt aggggccaac aaggcttcca 1140 gctggatgtg tgtgtagcat gtaccttatt atttttgtta ctgacagtta acagtggtgt 1200 gacatccaga gagcagctgg gctgctcccg ccccagcccg gcccagggtg aaggaagagg 1260 cacgtgctcc tcagagcagc cggagggagg ggggaggtcg gaggtcgtgg aggtggtttg 1320 tgtatcttac tggtctgaag ggaccaagtg tgtttgttgt ttgttttgta tcttgttttt 1380 ctgatcggag catcactact gacctgttgt aggcagctat cttacagacg catgaatgta 1440 agagtaggaa ggggtgggtg tcagggatca cttgggatct ttgacacttg aaaaattaca 1500 cctggcagct gcgtttaagc cttcccccat cgtgtactgc agagttgagc tggcagggga 1560 ggggctgaga gggtgggggc tggaacccct ccccgggagg agtgccatct gggtcttcca 1620 tctagaactg tttacatgaa gataagatac tcactgttca tgaatacact tgatgttcaa 1680 gtattaagac ctatgcaata ttttttactt ttctaataaa catgtttgtt aaaacaaaaa 1740 aaaa 1744 46 232 PRT Homo sapiens misc_feature Incyte ID No 3346307CD1 46 Met Pro Ser Leu Trp Asp Arg Phe Ser Ser Ser Ser Thr Ser Ser 1 5 10 15 Ser Pro Ser Ser Leu Pro Arg Thr Pro Thr Pro Asp Arg Pro Pro 20 25 30 Arg Ser Ala Trp Gly Ser Ala Thr Arg Glu Glu Gly Phe Asp Arg 35 40 45 Ser Thr Ser Leu Glu Ser Ser Asp Cys Glu Ser Leu Asp Ser Ser 50 55 60 Asn Ser Gly Phe Gly Pro Glu Glu Asp Thr Ala Tyr Leu Asp Gly 65 70 75 Val Ser Leu Pro Asp Phe Glu Leu Leu Ser Asp Pro Glu Asp Glu 80 85 90 His Leu Cys Ala Asn Leu Met Gln Leu Leu Gln Glu Ser Leu Ala 95 100 105 Gln Ala Arg Leu Gly Ser Arg Arg Pro Ala Arg Leu Leu Met Pro 110 115 120 Ser Gln Leu Val Ser Gln Val Gly Lys Glu Leu Leu Arg Leu Ala 125 130 135 Tyr Ser Glu Pro Cys Gly Leu Arg Gly Ala Leu Leu Asp Val Cys 140 145 150 Val Glu Gln Gly Lys Ser Cys His Ser Val Gly Gln Leu Ala Leu 155 160 165 Asp Pro Ser Leu Val Pro Thr Phe Gln Leu Thr Leu Val Leu Arg 170 175 180 Leu Asp Ser Arg Leu Trp Pro Lys Ile Gln Gly Leu Phe Ser Ser 185 190 195 Ala Asn Ser Pro Phe Leu Pro Gly Phe Ser Gln Ser Leu Thr Leu 200 205 210 Ser Thr Gly Phe Arg Val Ile Lys Lys Lys Leu Tyr Ser Ser Glu 215 220 225 Gln Leu Leu Ile Glu Glu Cys 230 47 897 DNA Homo sapiens misc_feature Incyte ID No 200143.25 47 ccccagggca gggagcaggt tatgaccagg actaaggtcc cagagtcccc accctgaccc 60 ctccctgctg ttccagccgc tccctcatat ccacccctgc cccatctcct gactttggtc 120 acgctagcat cttctgctga tcctgaaatt gtaccagcgg caagatgtgg cctggaaggg 180 gactttaagt tctccacaac tgccagcaat ccttccacca ggcaaaacac atcatctaag 240 gaaaagaagt gaggtcggaa caccaacgca tcatctcact gcatggccct ggaggctctg 300 ccgtttaaag accccagaac cttccccatt caaggtcctc tcctgggcac aggagattgg 360 agaaagctcc tcccttaatt ccagggaccg agttccagcc catccaattc tccgtctcac 420 ctgaggctgc tgtggtcctg gtgaccccag ggagcaacct gccgcccatg gctggggagg 480 gggtgaagct gtctctttaa gagcaggaat ggagcccctg ggcctcaggg catctgactt 540 gttttctacc tgcccaggtt tgcttagggc gtggcagctt cggataaacg caggactccg 600 cctggcagcc cgatttctcc cggaacctct gctcagcctg gtgaaccaca caggtgagca 660 gctggggccc cttcctccaa gccctccttg tctctgcccc taaattagga agtatctacc 720 tgccccctga ccctgcccca tagaagcttt tatgttaaag cgcctaaaat cttgtgaaat 780 gcttttctgg agccaggaga taaacggaag tcccttcccc taatgtccct ttccccacca 840 ttctcctctc agggacttgt tgaaccagct gaggccagcg ctctgacatg cagaagg 897 48 1827 DNA Homo sapiens misc_feature Incyte ID No 001929.1 48 ccttgacaat ctgtctgtcc gtctgcagct gcgtgactgt ctgtctctgc catgtctctc 60 tccccatgcc gggcccagag gggcttcagc gctcgctcag cctgttctgc tcgctcaagg 120 ggccgcagca ggggaggctt cagcagcagg ggcggcttca gcagcaggag ccttaattcc 180 tttggggggt gcctggaagg ctctcgtggg agtacctggg ggtcaggggg taggctgggg 240 gtgcggtttg gggagtggag tggtgggcct gggctctccc tgtgccctcc ggggggcatc 300 caagaagtga ccatcaacca gaatccgctg accccactga agattgagat cgatccccag 360 ttccaggtgg tgcggacgca ggagacccag gagatcagaa ccctcaacaa ccagtttgct 420 tccttcattg acaaggtgcg gttcctggag cagcagaaca aggtcctgga gacgaagtgg 480 catctgctgc agcaacaggg gttgagtggc agccagcagg gcctggagcc tgtctttgag 540 gcctgcctgg atcagctcag gaagcagctg gagcagctcc agggagaacg aggggctctg 600 gatgctgagt tgaaggcctg ccgggaccag gaggaggagt ataagtccaa gtatgaggag 660 gaggcccaca ggcgtgccac acttgagaac gactttgtgg tcctcaagaa ggatgtggat 720 ggggttttcc tgagcaagat ggagttggag ggcaagctgg aggctctgag agagtacctc 780 tacttcttga agcatctgaa tgaagaagag ctgggccagc tccagaccca ggccagcgac 840 acgtctgtgg tgctgtccat ggacaacaac cgctacctgg acttcagcag catcatcact 900 gaggtccgcg cccggtacga ggagatcgcc cggagcagca aggctgaggc tgaggccttg 960 taccagacca agtaccagga acttcaggtg tctgcccagc ttcatgggga caggatgcag 1020 gaaacgaaag tccagatctc tcagctacac caagagattc agaggctgca gagtcagact 1080 gagaacctca agaagcagaa cgccagcctg caggccgcca tcactgatgc tgagcagcgt 1140 ggggagctgg ccctcaagga cgctcaggcc aaggtggacg agctggaggc tgctctgagg 1200 atggccaagc agaacctggc ccggctgctg tgcgagtacc aggagctgac gagcacgaag 1260 ctttccctgg atgtggagat tgccacttac cgcaggctgc tggagggcga ggagtgcagg 1320 atgtctgggg agtgcaccag ccaggtcact atctcctcgg tgggaggcag cgctgtcatg 1380 tctggaggag ttggtggagg cttggggagc acttgtggac tcggtagtgg gaaaggcagc 1440 cctgggtcct gctgcaccag cattgtgact ggaggctcca acatcattct gggctctggg 1500 aaggaccctg ttttggattc ctgctctgtg tctggctcca gcgctggctc cagctgccac 1560 accatcctga agaagacagt tgagtcgagt ctgaagacat ccatcaccta ctgagcgacc 1620 cagcagccac ctccttcctg aacacatttg gcccactccc cccatcagcc ggctctgcaa 1680 ggccaactcc gtgtccgctg cccacagccc aagccagccc acagcggatg ctgcaaaaat 1740 caataaagtc tcccctcctg ctgttctgaa tgctctaagt gcttgcacac ctcacccagc 1800 aaaacaaaag ctgtgtgact ccccagc 1827 49 3936 DNA Homo sapiens misc_feature Incyte ID No 1088524.8 49 taaacacagc tgcgatgacg aaccctttca cgggaaggaa catgcgagcc cagaaaagtc 60 tctcctggtc ttgggatgga ggtcacacga agcctccgca aggcaaggac ttttgcggct 120 tctgcaacca agcgggtctt acccccggtc ctccgcgtct ccagtcctcg cacctggaac 180 cccaacgtcc ccgagagtcc ccgaatcccc gctcccaggc tacctaagag gatgagcggt 240 gctccgacgg ccggggcagc cctgatgctc tgcgccgcca ccgccgtgct actgagcgct 300 cagggcggac ccgtgcagtc caagtcgccg cgctttgcgt cctgggacga gatgaatgtc 360 ctggcgcacg gactcctgca gctcggccag gggctgcgcg aacacgcgga gcgcacccgc 420 agtcagctga gcgcgctgga gcggcgcctg agcgcgtgcg ggtccgcctg tcagggaacc 480 gaggggtcca ccgacctccc gttagcccct gagagccggg tggaccctga ggtccttcac 540 agcctgcaga cacaactcaa ggctcagaac agcaggatcc agcaactctt ccacaaggtg 600 gcccagcagc agcggcacct ggagaagcag cacctgcgaa ttcagcatct gcaaagccag 660 tttggcctcc tggaccacaa gcacctagac catgaggtgg ccaagcctgc ccgaagaaag 720 aggctgcccg agatggccca gccagttgac ccggctcaca atgtcagccg cctgcaccgg 780 ctgcccaggg attgccagga gctgttccag gttggggaga ggcagagtgg actatttgaa 840 atccagcctc aggggtctcc gccatttttg gtgaactgca agatgacctc agatggaggc 900 tggacagtaa ttcagaggcg ccacgatggc tcagtggact tcaaccggcc ctgggaagcc 960 tacaaggcgg ggtttgggga tccccacggc gagttctggc tgggtctgga gaaggtgcat 1020 agcatcaccg ggggaccgca acagccgcct ggccgtgcag ctgcgggact gggatggcaa 1080 cgccgagttg ctgcagttct ccgtgcacct gggtggcgag gacacggcct atagcctgca 1140 gctcactgca cccgtggccg gccagctggg cgccaccacc gtcccaccca gcggcctctc 1200 cgtacccttc tccacttggg accaggatca cgacctccgc agggacaaga actgcgccaa 1260 gagcctctct ggaggctggt ggtttggcac ctgcagccat tccaacctca acggccagta 1320 cttccgctcc atcccacagc agcggcagaa gcttaagaag ggaatcttct ggaagacctg 1380 gcggggccgc tactacccgc tgcaggccac caccatgttg atccagccca tggcagcaga 1440 ggcagcctcc tagcgtcctg gctgggcctg gtcccaggcc cacgaaagac ggtgactctt 1500 ggctctgccc gaggatgtgg ccgttccctg cctgggcagg ggctccaagg aggggccatc 1560 tggaaacttg tggacagaga agaagaccac gactggagaa gccccctttc tgagtgcagg 1620 ggggctgcat gcgttgcctc ctgagatcga ggctgcagga tatgctcaga ctctagaggc 1680 gtggaccaag gggcatggag cttcactcct tgctggccag ggagttgggg actcagaggg 1740 accacttggg gccagccaga ctggcctcaa tggcggactc agtcacattg actgacgggg 1800 accagggctt gtgtgggtcg agagcgccct catggtgctg gtgctgttgt gtgtaggtcc 1860 cctggggaca caagcaggcg ccaatggtat ctgggcggag ctcacagagt tcttggaata 1920 aaagcaacct cagaacactt tgttctttgt tcttgtttgt tttctttctt ttttttctct 1980 ttctttagtt cacagatcta gtaagttacc ctcagtttgt tttaaaaagt gaacaaagtc 2040 catgtaaaca tgttcccagn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn 2100 nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn 2160 nnnnnnnnnn catctcgcaa gggtccatgg cttcattctt gaagtcagtg agaccaagaa 2220 ccccccaatt ccggacacag tgccactgca ctccagccca ggcaacagag cgagattctg 2280 tctggacgta gccccatttc tcttcccgga caggtcctct gatagtcggg taggttctca 2340 atcaagcctc tcattagtta tttggtctgt caatccattt cattcctgca gtcttccgcc 2400 ccgccctctt gagctcgccc ctgataggct ggcgcgtccg tcacttcaaa aaggtccgca 2460 ttccttccgc ctttctccag gacaccgagg gcgaggaggg tggtaccaag cggcgcccac 2520 cctcagagca ctacttccat ctctgattgg cttcgctggg tgcccgtcgc tactccactc 2580 gccgatcccg ccggaagcgc caggacaatg gggacccggg acgacgagta cgactaccta 2640 ttcaaagtgg tgctcatcgg ggactcaggc gtgggcaaga gcaacctgct gtcgcgcttc 2700 acccgcaacg agttcaacct ggagagcaag agcaccatcg gcgtggagtt cgccacccgc 2760 agcatccagg tggacggcaa gaccatcaag gcgcagatct gggacaccgc tggccaggag 2820 cgctaccgcg ccatcacctc cgcgtactac cgtggtgcag tgggcgccct gctggtgtac 2880 gacatcgcca agcacctgac ctatgagaac gtggagcgct ggctgaagga gctgcgggac 2940 cacgcagaca gcaacatcgt catcatgctg gtgggcaaca agagtgacct gcgccacctg 3000 cgggctgtgc ccactgacga ggcccgcgcc ttcgcagaaa agaacaactt gtccttcatc 3060 gagacctcag ccttggattc cactaacgta gaggaagcat tcaagaacat cctcacagag 3120 atctaccgca tcgtgtcaca gaaacagatc gcagaccgtg ctgcccacga cgagtccccg 3180 gggaacaacg tggtggacat cagcgtgccg cccaccacgg acggacagaa gcccaacaag 3240 ctgcagtgct gccagaacct gtgacccctg cgcctccacc cagcgtgcgt gcacgtcctc 3300 cgcccgtccc cgccacggta tcctctggcc cctccctgct gtccctctgt ggccggctcg 3360 ttccagccct cccagtgagc tctgcacggc cgggccgggg cccaggaagg acaggagcca 3420 gtgctacccc gtcctgcccg gggaaaagct agaagccccg gtttgctgca cccatgaaac 3480 tcgggtcccc acagcgtctt ggcggggtgg ggagggcggc aggatggacg gggctggcca 3540 gaggcgagga ggacgggcgg acggcgccgc cttctcccct tttccttggc cgactctagg 3600 gagcgattgc ctccctccct ctgtgaccgg gtggcccagc cagcccgtcg tccccaccca 3660 gaaccgtgct ctgggccaaa gcccgaagaa ccaggcagcg ggggccgggg caggcggacc 3720 ccccgggctc tcagcgccca cccgctcctc cgcacacagc agctcgcaca ggcctcccac 3780 tctgcctgtc cccctnctnt gtctcgtctc cccatntggt ctggaacctg tttgcaagtg 3840 aagcaatatc tccgtgtttt gtagtataca accgctcttg tagcctttgg tttgtgttaa 3900 tgtagagaaa ctcagattct ttatacactt ttgtaa 3936 50 1114 DNA Homo sapiens misc_feature Incyte ID No 632664CB1 50 gccgcctctg ccgccgcgga cttcccgaac ctcttcagcc gcccggagcc gctcccggag 60 cccggccgta gaggctgcaa tcgcagccgg tgagcccgca gcccgcgccc cgagcccgcc 120 gccgcccttc gagggcgccc caggccgcgc catggtgaag gtgacgttca actccgctct 180 ggcccagaag gaggccaaga aggacgagcc caagagcggc gaggaggcgc tcatcatccc 240 ccccgacgcc gtcgcggtgg actgcaagga cccagatgat gtggtaccag ttggccaaag 300 aagagcctgg tgttggtgca tgtgctttgg actagcattt atgcttgcag gtgttattct 360 aggaggagca tacttgtaca aatattttgc acttcaacca gatgacgtgt actactgtgg 420 aataaagtac atcaaagatg atgtcatctt aaatgagccc tctgcagatg ccccagctgc 480 tctctaccag acaattgaag aaaatattaa aatctttgaa gaagaagaag ttgaatttat 540 cagtgtgcct gtcccagagt ttgcagatag tgatcctgcc aacattgttc atgactttaa 600 caagaaactt acagcctatt tagatcttaa cctggataag tgctatgtga tccctctgaa 660 cacttccatt gttatgccac ccagaaacct actggagtta cttattaaca tcaaggctgg 720 aacctatttg cctcagtcct atctgattca tgagcacatg gttattactg atcgcattga 780 aaacattgat cacctgggtt tctttattta tcgactgtgt catgacaagg aaacttacaa 840 actgcaacgc agagaaacta ttaaaggtat tcagaaacgt gaagccagca attgtttcgc 900 aattcggcat tttgaaaaca aatttgccgt ggaaacttta atttgttctt gaacagtcaa 960 gaaaaacatt attgaggaaa attaatatca cagcataacc ccacccttta cattttgtgc 1020 agtgattatt ttttaaagtc ttctttcatg taagtagcaa acagggcttt actatctttt 1080 catctcatta attcaattaa aaccattacc ttaa 1114 51 266 PRT Homo sapiens misc_feature Incyte ID No 632664CD1 51 Met Val Lys Val Thr Phe Asn Ser Ala Leu Ala Gln Lys Glu Ala 1 5 10 15 Lys Lys Asp Glu Pro Lys Ser Gly Glu Glu Ala Leu Ile Ile Pro 20 25 30 Pro Asp Ala Val Ala Val Asp Cys Lys Asp Pro Asp Asp Val Val 35 40 45 Pro Val Gly Gln Arg Arg Ala Trp Cys Trp Cys Met Cys Phe Gly 50 55 60 Leu Ala Phe Met Leu Ala Gly Val Ile Leu Gly Gly Ala Tyr Leu 65 70 75 Tyr Lys Tyr Phe Ala Leu Gln Pro Asp Asp Val Tyr Tyr Cys Gly 80 85 90 Ile Lys Tyr Ile Lys Asp Asp Val Ile Leu Asn Glu Pro Ser Ala 95 100 105 Asp Ala Pro Ala Ala Leu Tyr Gln Thr Ile Glu Glu Asn Ile Lys 110 115 120 Ile Phe Glu Glu Glu Glu Val Glu Phe Ile Ser Val Pro Val Pro 125 130 135 Glu Phe Ala Asp Ser Asp Pro Ala Asn Ile Val His Asp Phe Asn 140 145 150 Lys Lys Leu Thr Ala Tyr Leu Asp Leu Asn Leu Asp Lys Cys Tyr 155 160 165 Val Ile Pro Leu Asn Thr Ser Ile Val Met Pro Pro Arg Asn Leu 170 175 180 Leu Glu Leu Leu Ile Asn Ile Lys Ala Gly Thr Tyr Leu Pro Gln 185 190 195 Ser Tyr Leu Ile His Glu His Met Val Ile Thr Asp Arg Ile Glu 200 205 210 Asn Ile Asp His Leu Gly Phe Phe Ile Tyr Arg Leu Cys His Asp 215 220 225 Lys Glu Thr Tyr Lys Leu Gln Arg Arg Glu Thr Ile Lys Gly Ile 230 235 240 Gln Lys Arg Glu Ala Ser Asn Cys Phe Ala Ile Arg His Phe Glu 245 250 255 Asn Lys Phe Ala Val Glu Thr Leu Ile Cys Ser 260 265 52 1189 DNA Homo sapiens misc_feature Incyte ID No 457372.17 52 acaggtgtga gccaccacac ccagcagttt ttttaaggtc acaaaatgac aagactagga 60 tttggaccca gttctgttcg actcaaaata gagtgcccta cacttatgtg tcatgctgca 120 tttggcaagt cacgtcactt ctttgaatct ccttttccct ctgcaaaaca gtaaccttat 180 ctagcctgca gacttcaaag gtggttatgg agatcaaatg aagtaaaatg ttttaaaaat 240 tgtacaatat ataccaataa aagctattgg ggaggtatat gtatgaacag gtagttggtt 300 tttctaccct gccacctcat aaagagtttg cagtggcacg tagaagggtt tatcttatta 360 tcacaaagct acccatttgc tggccatact gatacttggc acattaaact atcagagaaa 420 tatatgtggc tcctttacaa ctgtgtctag aagggtacat ttccaatcag agttcccagg 480 ttctgacttt ctcccattac atatttgtaa ttagtcatct ttgatactga ttcaaatttt 540 tgattaacat taattatata tatttacaag aatcttataa aaattaagat tttatttcac 600 ctcattttgc cctgtgagat agatggaaat agactatatt ctacccaggt taaaagtaca 660 gataatgaga caaaatgtca atagaacctg aaaaaagatt tttttagttg cctctagtct 720 ctgtttactt ggtatagata gtatgctgct tttttttctt ttttttaaaa tgtaactgct 780 gggttgtttt ttttttcttg ttttttcttt ccctccagga tacaatgtct ctttgctata 840 tgaccttgaa aatcttccgg catccaagga ttccattgtg catcaagctg gcatgttgaa 900 gcgaaattgt tttgcctctg tctttgaaaa atacttccaa ttccaagaag agggcaagga 960 aggagagaac agggcagtta tccattatag ggatgatgag accatgtatg ttgagtctaa 1020 aaaggacaga gtcacagtag tcttcagcac agtgtttaag gatgacgacg atgtggtcat 1080 tggaaaggtg ttcatgcagg tatggagcag acatcttggg ggaaacccat gcatggcgac 1140 ttataccttt gcacccaaac ataccatgag cgtaggaaag agatctagc 1189 53 2539 DNA Homo sapiens misc_feature Incyte ID No 2993696CB1 53 ctcgagccgc aagacagcac agacagattg acctattggg gtgtttcgcg agtgtgagag 60 ggaagcgccg cggcctgtat ttctagacct gcccttcgcc tggttcgtgg cgccttgtga 120 ccccgggccc ctgccgcctg caagtcggaa attgcgctgt gctcctgtgc tacggcctgt 180 ggctggactg cctgctgctg cccaactggc tggcaagatg aagctctccc tggtggccgc 240 gatgctgctg ctgctcagcg cggcgcgggc cgaggaggag gacaagaagg aggacgtggg 300 cacggtggtc ggcatcgacc tggggaccac ctactcctgc gtcggcgtgt tcaagaacgg 360 ccgcgtggag atcatcgcca acgatcaggg caaccgcatc acgccgtcct atgtcgcctt 420 cactcctgaa ggggaacgtc tgattggcga tgccgccaag aaccagctca cctccaaccc 480 cgagaacacg gtctttgacg ccaagcggct catcggccgc acgtggaatg acccgtctgt 540 gcagcaggac atcaagttct tgccgttcaa ggtggttgaa aagaaaacta aaccatacat 600 tcaagttgat attggaggtg ggcaaacaaa gacatttgct cctgaagaaa tttctgccat 660 ggttctcact aaaatgaaag aaaccgctga ggcttatttg ggaaagaagg ttacccatgc 720 agttgttact gtaccagcct attttaatga tgcccaacgc caagcaacca aagacgctgg 780 aactattgct ggcctaaatg ttatgaggat catcaacgag cctacggcag ctgctattgc 840 ttatggcctg gataagaggg agggggagaa gaacatcctg gtgtttgacc tgggtggcgg 900 aaccttcgat gtgtctcttc tcaccattga caatggtgtc ttcgaagttg tggccactaa 960 tggagatact catctgggtg gagaagactt tgaccagcgt gtcatggaac acttcatcaa 1020 actgtacaaa aagaagacgg gcaaagatgt caggaaagac aatagagctg tgcagaaact 1080 ccggcgcgag gtagaaaagg ccaaacgggc cctgtcttct cagcatcaag caagaattga 1140 aattgagtcc ttctatgaag gagaagactt ttctgagacc ctgactcggg ccaaatttga 1200 agagctcaac atggatctgt tccggtctac tatgaagccc gtccagaaag tgttggaaga 1260 ttctgatttg aagaagtctg atattgatga aattgttctt gttggtggct cgactcgaat 1320 tccaaagatt cagcaactgg ttaaagagtt cttcaatggc aaggaaccat cccgtggcat 1380 aaacccagat gaagctgtag cgtatggtgc tgctgtccag gctggtgtgc tctctggtga 1440 tcaagataca ggtgacctgg tactgcttga tgtatgtccc cttacacttg gtattgaaac 1500 tgtgggaggt gtcatgacca aactgattcc aaggaacaca gtggtgccta ccaagaagtc 1560 tcagatcttt tctacagctt ctgataatca accaactgtt acaatcaagg tctatgaagg 1620 tgaaagaccc ctgacaaaag acaatcatct tctgggtaca tttgatctga ctggaattcc 1680 tcctgctcct cgtggggtcc cacagattga agtcaccttt gagatagatg tgaatggtat 1740 tcttcgagtg acagctgaag acaagggtac agggaacaaa aataagatca caatcaccaa 1800 tgaccagaat cgcctgacac ctgaagaaat cgaaaggatg gttaatgatg ctgagaagtt 1860 tgctgaggaa gacaaaaagc tcaaggagcg cattgatact agaaatgagt tggaaagcta 1920 tgcctattct ctaaagaatc agattggaga taaagaaaag ctgggaggta aactttcctc 1980 tgaagataag gagaccatgg aaaaagctgt agaagaaaag attgaatggc tggaaagcca 2040 ccaagatgct gacattgaag acttcaaagc taagaagaag gaactggaag aaattgttca 2100 accaattatc agcaaactct atggaagtgc aggccctccc ccaactggtg aagaggatac 2160 agcagaaaaa gatgagttgt agacactgat ctgctagtgc tgtaatattg taaatactgg 2220 actcaggaac ttttgttagg aaaaaattga aagaacttaa gtctcgaatg taattggaat 2280 cttcacctca gagtggagtt gaaactgcta tagcctaagc ggctgtttac tgcttttcat 2340 tagcagttgc tcacatgtct ttgggtgggg gggagaagaa gaattggcca tcttaaaaag 2400 cgggtaaaaa acctgggtta gggtgtgtgt tcaccttcaa aatgttctat ttaacaactg 2460 ggtcatgtgc atctggtgta ggaagttttt tctaccataa gtgacaccaa taaatgtttg 2520 ttatttacac tggtaagcg 2539 54 654 PRT Homo sapiens misc_feature Incyte ID No 2993696CD1 54 Met Lys Leu Ser Leu Val Ala Ala Met Leu Leu Leu Leu Ser Ala 1 5 10 15 Ala Arg Ala Glu Glu Glu Asp Lys Lys Glu Asp Val Gly Thr Val 20 25 30 Val Gly Ile Asp Leu Gly Thr Thr Tyr Ser Cys Val Gly Val Phe 35 40 45 Lys Asn Gly Arg Val Glu Ile Ile Ala Asn Asp Gln Gly Asn Arg 50 55 60 Ile Thr Pro Ser Tyr Val Ala Phe Thr Pro Glu Gly Glu Arg Leu 65 70 75 Ile Gly Asp Ala Ala Lys Asn Gln Leu Thr Ser Asn Pro Glu Asn 80 85 90 Thr Val Phe Asp Ala Lys Arg Leu Ile Gly Arg Thr Trp Asn Asp 95 100 105 Pro Ser Val Gln Gln Asp Ile Lys Phe Leu Pro Phe Lys Val Val 110 115 120 Glu Lys Lys Thr Lys Pro Tyr Ile Gln Val Asp Ile Gly Gly Gly 125 130 135 Gln Thr Lys Thr Phe Ala Pro Glu Glu Ile Ser Ala Met Val Leu 140 145 150 Thr Lys Met Lys Glu Thr Ala Glu Ala Tyr Leu Gly Lys Lys Val 155 160 165 Thr His Ala Val Val Thr Val Pro Ala Tyr Phe Asn Asp Ala Gln 170 175 180 Arg Gln Ala Thr Lys Asp Ala Gly Thr Ile Ala Gly Leu Asn Val 185 190 195 Met Arg Ile Ile Asn Glu Pro Thr Ala Ala Ala Ile Ala Tyr Gly 200 205 210 Leu Asp Lys Arg Glu Gly Glu Lys Asn Ile Leu Val Phe Asp Leu 215 220 225 Gly Gly Gly Thr Phe Asp Val Ser Leu Leu Thr Ile Asp Asn Gly 230 235 240 Val Phe Glu Val Val Ala Thr Asn Gly Asp Thr His Leu Gly Gly 245 250 255 Glu Asp Phe Asp Gln Arg Val Met Glu His Phe Ile Lys Leu Tyr 260 265 270 Lys Lys Lys Thr Gly Lys Asp Val Arg Lys Asp Asn Arg Ala Val 275 280 285 Gln Lys Leu Arg Arg Glu Val Glu Lys Ala Lys Arg Ala Leu Ser 290 295 300 Ser Gln His Gln Ala Arg Ile Glu Ile Glu Ser Phe Tyr Glu Gly 305 310 315 Glu Asp Phe Ser Glu Thr Leu Thr Arg Ala Lys Phe Glu Glu Leu 320 325 330 Asn Met Asp Leu Phe Arg Ser Thr Met Lys Pro Val Gln Lys Val 335 340 345 Leu Glu Asp Ser Asp Leu Lys Lys Ser Asp Ile Asp Glu Ile Val 350 355 360 Leu Val Gly Gly Ser Thr Arg Ile Pro Lys Ile Gln Gln Leu Val 365 370 375 Lys Glu Phe Phe Asn Gly Lys Glu Pro Ser Arg Gly Ile Asn Pro 380 385 390 Asp Glu Ala Val Ala Tyr Gly Ala Ala Val Gln Ala Gly Val Leu 395 400 405 Ser Gly Asp Gln Asp Thr Gly Asp Leu Val Leu Leu Asp Val Cys 410 415 420 Pro Leu Thr Leu Gly Ile Glu Thr Val Gly Gly Val Met Thr Lys 425 430 435 Leu Ile Pro Arg Asn Thr Val Val Pro Thr Lys Lys Ser Gln Ile 440 445 450 Phe Ser Thr Ala Ser Asp Asn Gln Pro Thr Val Thr Ile Lys Val 455 460 465 Tyr Glu Gly Glu Arg Pro Leu Thr Lys Asp Asn His Leu Leu Gly 470 475 480 Thr Phe Asp Leu Thr Gly Ile Pro Pro Ala Pro Arg Gly Val Pro 485 490 495 Gln Ile Glu Val Thr Phe Glu Ile Asp Val Asn Gly Ile Leu Arg 500 505 510 Val Thr Ala Glu Asp Lys Gly Thr Gly Asn Lys Asn Lys Ile Thr 515 520 525 Ile Thr Asn Asp Gln Asn Arg Leu Thr Pro Glu Glu Ile Glu Arg 530 535 540 Met Val Asn Asp Ala Glu Lys Phe Ala Glu Glu Asp Lys Lys Leu 545 550 555 Lys Glu Arg Ile Asp Thr Arg Asn Glu Leu Glu Ser Tyr Ala Tyr 560 565 570 Ser Leu Lys Asn Gln Ile Gly Asp Lys Glu Lys Leu Gly Gly Lys 575 580 585 Leu Ser Ser Glu Asp Lys Glu Thr Met Glu Lys Ala Val Glu Glu 590 595 600 Lys Ile Glu Trp Leu Glu Ser His Gln Asp Ala Asp Ile Glu Asp 605 610 615 Phe Lys Ala Lys Lys Lys Glu Leu Glu Glu Ile Val Gln Pro Ile 620 625 630 Ile Ser Lys Leu Tyr Gly Ser Ala Gly Pro Pro Pro Thr Gly Glu 635 640 645 Glu Asp Thr Ala Glu Lys Asp Glu Leu 650 55 5762 DNA Homo sapiens misc_feature Incyte ID No 331106.6 55 gcgcgaccgt cccgggggtg gggccgggcg cagcggcgag aggaggcgaa ggtggctgcg 60 gtagcagcag cgcggcagcc tcgtgaccca gcccggagcg cagggcggcc gctgcaggtc 120 cccgctcccc tccccgtgcg tccgcccatg gccgccgccg ggcagctgtg cttgctctac 180 ctgtcggcgg ggctcctgtc ccggctcggc gcagccttca acttggacac tcgggaggac 240 aacgtgatcc ggaaatatgg agaccccggg agcctcttcg gcttctcgct ggccatgcac 300 tggcaactgc agcccgagga caagcggctg ttgctcgtgg gggccccgcg ggcagaagcg 360 cttccactgc agagagccaa cagaacggga gggctgtaca gctgcgacat caccgcccgg 420 gggccatgca cgcggatcga gtttgataac gatgctgacc ccacgtcaga aagcaaggaa 480 gatcagtgga tgggggtcac cgtccagagc caaggtccag ggggcaaggt cgtgacatgt 540 gctcaccgat atgaaaaaag gcagcatgtt aatacgaagc aggaatcccg agacatcttt 600 gggcggtgtt atgtcctgag tcagaatctc aggattgaag acgatatgga tgggggagat 660 tggagctttt gtgatgggcg attgagaggc catgagaaat ttggctcttg ccagcaaggt 720 gtagcagcta cttttactaa agactttcat tacattgtat ttggagcccc gggtacttat 780 aactggaaag ggattgttcg tgtagagcaa aagaataaca ctttttttga catgaacatc 840 tttgaagatg ggccttatga agttggtgga gagactgagc atgatgaaag tctcgttcct 900 gttcctgcta acagttactt aggtttttct ttggactcag ggaaaggtat tgtttctaaa 960 gatgagatca cttttgtatc tggtgctccc agagccaatc acagtggagc cgtggttttg 1020 ctgaagagag acatgaagtc tgcacatctc ctccctgagc acatattcga tggagaaggt 1080 ctggcctctt catttggcta tgatgtggcg gtggtggacc tcaacaagga tgggtggcaa 1140 gatatagtta ttggagcccc acagtatttt gatagagatg gagaagttgg aggtgcagtg 1200 tatgtctaca tgaaccagca aggcagatgg aataatgtga agccaattcg tcttaatgga 1260 accaaagatt ctatgtttgg cattgcagta aaaaatattg gagatattaa tcaagatggc 1320 tacccagata ttgcagttgg agctccgtat gatgacttgg gaaaggtttt tatctatcat 1380 ggatctgcaa atggaataaa taccaaacca acacaggttc tcaagggtat atcaccttat 1440 tttggatatt caattgctgg aaacatggac cttgatcgaa attcctaccc tgatgttgct 1500 gttggttccc tctcagattc agtaactatt ttcagatccc ggcctgtgat taatattcag 1560 aaaaccatca cagtaactcc taacagaatt gacctccgcc agaaaacagc gtgtggggcg 1620 cctagtggga tatgcctcca ggttaaatcc tgttttgaat atactgctaa ccccgctggt 1680 tataatcctt caatatcaat tgtgggcaca cttgaagctg aaaaagaaag aagaaaatct 1740 gggctatcct caagagttca gtttcgaaac caaggttctg agcccaaata tactcaagaa 1800 ctaactctga agaggcagaa acagaaagtg tgcatggagg aaaccctgtg gctacaggat 1860 aatatcagag ataaactgcg tcccattccc ataactgcct cagtggagat ccaagagcca 1920 agctctcgta ggcgagtgaa ttcacttcca gaagttcttc caattctgaa ttcagatgaa 1980 cccaagacag ctcatattga tgttcacttc ttaaaagagg gatgtggaga cgacaatgta 2040 tgtaacagca accttaaact agaatataaa ttttgcaccc gagaaggaaa tcaagacaaa 2100 ttttcttatt taccaattca aaaaggtgta ccagaactag ttctaaaaga tcagaaggat 2160 attgctttag aaataacagt gacaaacagc ccttccaacc caaggaatcc cacaaaagat 2220 ggcgatgacg cccatgaggc taaactgatt gcaacgtttc cagacacttt aacctattct 2280 gcatatagag aactgagggc tttccctgag aaacagttga gttgtgttgc caaccagaat 2340 ggctcgcaag ctgactgtga gctcggaaat ccttttaaaa gaaattcaaa tgtcactttt 2400 tatttggttt taagtacaac tgaagtcacc tttgacaccc cagatctgga tattaatctg 2460 aagttagaaa caacaagcaa tcaagataat ttggctccaa ttacagctaa agcaaaagtg 2520 gttattgaac tgcttttatc ggtctcggga gttgctaaac cttcccaggt gtattttgga 2580 ggtacagttg ttggcgagca agctatgaaa tctgaagatg aagtgggaag tttaatagag 2640 tatgaattca gggtaataaa cttaggtaaa cctcttacaa acctcggcac agcaaccttg 2700 aacattcagt ggccaaaaga aattagcaat gggaaatggt tgctttattt ggtgaaagta 2760 gaatccaaag gattggaaaa ggtaacttgt gagccacaaa aggagataaa ctccctgaac 2820 ctaacggagt ctcacaactc aagaaagaaa cgggaaatta ctgaaaaaca gatagatgat 2880 aacagaaaat tttctttatt tgctgaaaga aaataccaga ctcttaactg tagcgtgaac 2940 gtgaactgtg tgaacatcag atgcccgctg cgggggctgg acagcaaggc gtctcttatt 3000 ttgcgctcga ggttatggaa cagcacattt ctagaggaat attccaaact gaactacttg 3060 gacattctca tgcgagcctt cattgatgtg actgctgctg ccgaaaatat caggctgcca 3120 aatgcaggca ctcaggttcg agtgactgtg tttccctcaa agactgtagc tcagtattcg 3180 ggagtacctt ggtggatcat cctagtggct attctcgctg ggatcttgat gcttgcttta 3240 ttagtgttta tactatggaa gtgtggtttc ttcaagagaa ataagaaaga tcattatgat 3300 gccacatatc acaaggctga gatccatgct cagccatctg ataaagagag gcttacttct 3360 gatgcatagt attgatctac ttctgtaatt gtgtggattc tttaaacgct ctaggtacga 3420 tgacagtgtt ccccgatacc atgctgtaag gatccggaaa gaagagcgag agatcaaaga 3480 tgaaaagtat attgataacc ttgaaaaaaa acagtggatc acaaagtgga acagaaatga 3540 aagctactca tagcgggggc ctaaaaaaaa aaaaagcttc acagtaccca aactgctttt 3600 tccaactcag aaattcaatt tggatttaaa agcctgctca atccctgagg actgatttca 3660 gagtgactac acacagtacg aacctacagt tttaactgtg gatattgtta cgtagcctaa 3720 ggctcctgtt ttgcacagcc aaatttaaaa ctgttggaat ggatttttct ttaactgccg 3780 taatttaact ttctgggttg cctttgtttt tggcgtggct gacttacatc atgtgttggg 3840 gaagggcctg cccagttgca ctcaggtgac atcctccaga tagtgtagct gaggaggcac 3900 ctacactcac ctgcactaac agagtggccg tcctaacctc gggcctgctg cgcagacgtc 3960 catcacgtta gctgtcccac atcacaagac tatgccattg gggtagttgt gtttcaacgg 4020 aaagtgctgt cttaaactaa atgtgcaata gaaggtgatg ttgccatcct accgtctttt 4080 cctgtttcct agctgtgtga atacctgctc acgtcaaatg catacaagtt tcattctccc 4140 tttcactaaa aacacacagg tgcaacagac ttgaatgcta gttatactta tttgtatatg 4200 gtatttattt tttcttttct ttacaaacca ttttgttatt gactaacagg ccaaagagtc 4260 tccagtttac ccttcaggtt ggtttaatca atcagaatta gaattagagc atgggaggtc 4320 atcactttga cctaaattat ttactgcaaa aagaaaatct ttataaatgt accagagaga 4380 gttgttttaa taacttatct ataaactata acctctcctt catgacagcc tccaccccac 4440 aacccaaaag gtttaagaaa tagaattata actgtaaaga tgtttatttc aggcattgga 4500 tattttttac tttagaagcc tgcataatgt ttctggattt catactgtaa cattcaggaa 4560 ttcttggaga aaatgggttt attcactgaa ctctagtgcg gtttactcac tgctgcaaat 4620 actgtatatt caggacttga aagaaatggt gaatgcctat ggtggatcca aactgatcca 4680 gtataagact actgaatctg ctaccaaaac agttaatcag tgagtcgatg ttctattttt 4740 tgttttgttt cctcccctat ctgtattccc aaaaattact ttggggctaa tttaacaaga 4800 actttaaatt gtgttttaat tgtaaaaatg gcagggggtg gaattattac tctatacatt 4860 caacagagac tgaatagata tgaaagctga ttttttttaa ttaccatgct tcacaatgtt 4920 aagttatatg gggagcaaca gcaaacaggt gctaatttgt tttggatata gtataagcag 4980 tgtctgtgtt ttgaaagaat agaacacagt ttgtagtgcc actgttgttt tgggggggct 5040 tttttctttt cggaaatctt aaaccttaag atactaagga cgttgttttg gttgtacttt 5100 ggaattctta gtcacaaaat atattttgtt tacaaaaatt tctgtaaaac aggttataac 5160 agtgtttaaa gtctcagttt cttgcttggg gaacttgtgt ccctaatgtg tttagattgc 5220 tagattgcta aggagctgat actttgacag tgtttttaga cctgtgttac taaaaaaaag 5280 atgaatgtcc tgaaaagggt gttgggaggg tggttcaaca aagaaacaaa gatgttatgg 5340 tgtttagatt tatggttgtt aaaaatgtca tctcaagtca agtcactggt ctgtttgcat 5400 ttgatacatt tttgtactaa ctagcattgt aaaattattt catgattaga aattacctgt 5460 ggatatttgt ataaaagtgt gaaataaatt ttttataaaa gtgttcattg tttcgtaaca 5520 cagcattgta tatgtgaagc aaactctaaa attataaatg acaacctgaa ttatctattt 5580 catcaaacca aagttcagtg tttttatttt tggtgtctca tgtaatctca gatcagccaa 5640 agatactagt gccaaagcaa tgggattcgg ggtttttttc tgttttcgct ctatgtaggt 5700 gatcctcaag tctttcattt tccttcttta tgattaaaag aaacctacag gtatttaaca 5760 ac 5762 56 2471 DNA Homo sapiens misc_feature Incyte ID No 1256895CB1 56 ccgcgcgtcg cctgtcctcc gagccagtcg ctgacagccg cggcgccgcg agcttctcct 60 ctcctcacga ccgaggcaga gcagtcatta tggcgaacct tggctgctgg atgctggttc 120 tctttgtggc cacatggagt gacctgggcc tctgcaagaa gcgcccgaag cctggaggat 180 ggaacactgg gggcagccga tacccggggc agggcagccc tggaggcaac cgctacccac 240 ctcagggcgg tggtggctgg gggcagcctc atggtggtgg ctgggggcag cctcatggtg 300 gtggctgggg gcagccccat ggtggtggct ggggacagcc tcatggtggt ggctggggtc 360 aaggaggtgg cacccacagt cagtggaaca agccgagtaa gccaaaaacc aacatgaagc 420 acatggctgg tgctgcagca gctggggcag tggtgggggg ccttggcggc tacgtgctgg 480 gaagtgccat gagcaggccc atcatacatt tcggcagtga ctatgaggac cgttactatc 540 gtgaaaacat gcaccgttac cccaaccaag tgtactacag gcccatggat gagtacagca 600 accagaacaa ctttgtgcac gactgcgtca atatcacaat caagcagcac acggtcacca 660 caaccaccaa gggggagaac ttcaccgaga ccgacgttaa gatgatggag cgcgtggttg 720 agcagatgtg tatcacccag tacgagaggg aatctcaggc ctattaccag agaggatcga 780 gcatggtcct cttctcctct ccacctgtga tcctcctgat ctctttcctc atcttcctga 840 tagtgggatg aggaaggtct tcctgttttc accatctttc taatcttttt ccagcttgag 900 ggaggcggta tccacctgca gcccttttag tggtggtgtc tcactctttc ttctctcttt 960 gtcccggata ggctaatcaa tacccttggc actgatgggc actggaaaac atagagtaga 1020 cctgagatgc tggtcaagcc ccctttgatt gagttcatca tgagccgttg ctaatgccag 1080 gccagtaaaa gtataacagc aaataaccat tggttaatct ggacttattt ttggacttag 1140 tgcaacaggt tgaggctaaa acaaatctca gaacagtctg aaataccttt gcctggatac 1200 ctctggctcc ttcagcagct agagctcagt atactaatgc cctatcttag tagagatttc 1260 atagctattt agagatattt tccattttaa gaaaacccga caacatttct gccaggtttg 1320 ttaggaggcc acatgatact tattcaaaaa aatcctagag attcttagct cttgggatgc 1380 aggctcagcc cgctggagca tgagctctgt gtgtaccgag aactggggtg atgttttact 1440 tttcacagta tgggctacac agcagctgtt caacaagagt aaatattgtc acaacactga 1500 acctctggct agaggacata ttcacagtga acataactgt aacatatatg aaaggcttct 1560 gggacttgaa atcaaatgtt tgggaatggt gcccttggag gcaacctccc attttagatg 1620 tttaaaggac cctatatgtg gcattccttt ctttaaacta taggtaatta aggcagctga 1680 aaagtaaatt gccttctaga cactgaaggc aaatctcctt tgtccattta cctggaaacc 1740 agaatgattt tgacatacag gagagctgca gttgtgaaag caccatcatc atagaggatg 1800 atgtaattaa aaaatggtca gtgtgcaaag aaaagaactg cttgcatttc tttatttctg 1860 tctcataatt gtcaaaaacc agaattaggt caagttcata gtttctgtaa ttggcttttg 1920 aatcaaagaa tagggagaca atctaaaaaa tatcttaggt tggagatgac agaaatatga 1980 ttgatttgaa gtggaaaaag aaattctgtt aatgttaatt aaagtaaaat tattccctga 2040 attgtttgat attgtcacct agcagatatg tattactttt ctgcaatgtt attattggct 2100 tgcactttgt gagtattcta tgtaaaaata tatatgtata taaaatatat attgcatagg 2160 acagacttag gagttttgtt tagagcagtt aacatctgaa gtgtctaatg cattaacttt 2220 tgtaaggtac tgaatactta atatgtggga aacccttttg cgtggtcctt aggcttacaa 2280 tgtgcactga atcgtttcat gtaagaatcc aaagtggaca ccattaacag gtctttgaaa 2340 tatgcatgta ctttatattt tctatatttg taactttgca tgttcttgtt ttgttatata 2400 aaaaaattgt aaatgtttaa tatctgactg aaattaaacg agcgaagatg agcaccaaaa 2460 aaaaaaaaaa a 2471 57 253 PRT Homo sapiens misc_feature Incyte ID No 1256895CD1 57 Met Ala Asn Leu Gly Cys Trp Met Leu Val Leu Phe Val Ala Thr 1 5 10 15 Trp Ser Asp Leu Gly Leu Cys Lys Lys Arg Pro Lys Pro Gly Gly 20 25 30 Trp Asn Thr Gly Gly Ser Arg Tyr Pro Gly Gln Gly Ser Pro Gly 35 40 45 Gly Asn Arg Tyr Pro Pro Gln Gly Gly Gly Gly Trp Gly Gln Pro 50 55 60 His Gly Gly Gly Trp Gly Gln Pro His Gly Gly Gly Trp Gly Gln 65 70 75 Pro His Gly Gly Gly Trp Gly Gln Pro His Gly Gly Gly Trp Gly 80 85 90 Gln Gly Gly Gly Thr His Ser Gln Trp Asn Lys Pro Ser Lys Pro 95 100 105 Lys Thr Asn Met Lys His Met Ala Gly Ala Ala Ala Ala Gly Ala 110 115 120 Val Val Gly Gly Leu Gly Gly Tyr Val Leu Gly Ser Ala Met Ser 125 130 135 Arg Pro Ile Ile His Phe Gly Ser Asp Tyr Glu Asp Arg Tyr Tyr 140 145 150 Arg Glu Asn Met His Arg Tyr Pro Asn Gln Val Tyr Tyr Arg Pro 155 160 165 Met Asp Glu Tyr Ser Asn Gln Asn Asn Phe Val His Asp Cys Val 170 175 180 Asn Ile Thr Ile Lys Gln His Thr Val Thr Thr Thr Thr Lys Gly 185 190 195 Glu Asn Phe Thr Glu Thr Asp Val Lys Met Met Glu Arg Val Val 200 205 210 Glu Gln Met Cys Ile Thr Gln Tyr Glu Arg Glu Ser Gln Ala Tyr 215 220 225 Tyr Gln Arg Gly Ser Ser Met Val Leu Phe Ser Ser Pro Pro Val 230 235 240 Ile Leu Leu Ile Ser Phe Leu Ile Phe Leu Ile Val Gly 245 250 58 5681 DNA Homo sapiens misc_feature Incyte ID No 474630.29 58 cccgcgcccg ccctcggaca gtccctgctc gcccgcgcgc tgcagcccca tctcctagcg 60 gcagcccagg cgcggaggga gcgagtccgc cccgaggtag gtccaggacg ggcgcacagc 120 agcagccgag gctggccggg agagggagga agaggatggc agggccacgc cccagcccat 180 gggccaggct gctcctggca gccttgatca gcgtcagcct ctctgggacc ttggcaaacc 240 gctgcaagaa ggccccagtg aagagctgca cggagtgtgt ccgtgtggat aaggactgcg 300 cctactgcac agacgagatg ttcagggacc ggcgctgcaa cacccaggcg gagctgctgg 360 ccgcgggctg ccagcgggag agcatcgtgg tcatggagag cagcttccaa atcacagagg 420 agacccagat tgacaccacc ctgcggcgca gccagatgtc cccccaaggc ctgcgggtcc 480 gtctgcggcc cggtgaggag cggcattttg agctggaggt gtttgagcca ctggagagcc 540 ccgtggacct gtacatcctc atggacttct ccaactccat gtccgatgat ctggacaacc 600 tcaagaagat ggggcagaac ctggctcggg tcctgagcca gctcaccagc gactacacta 660 ttggatttgg caagtttgtg gacaaagtca gcgtcccgca gacggacatg aggcctgaga 720 agctgaagga gccctggccc aacagtgacc cccccttctc cttcaagaac gtcatcagcc 780 tgacagaaga tgtggatgag ttccggaata aactgcaggg agagcggatc tcaggcaacc 840 tggatgctcc tgagggcggc ttcgatgcca tcctgcagac agctgtgtgc acgagggaca 900 ttggctggcg cccggacagc acccacctgc tggtcttctc caccgagtca gccttccact 960 atgaggctga tggcgccaac gtgctggctg gcatcatgag ccgcaacgat gaacggtgcc 1020 acctggacac cacgggcacc tacacccagt acaggacaca ggactacccg tcggtgccca 1080 ccctggtgcg cctgctcgcc aagcacaaca tcatccccat ctttgctgtc accaactact 1140 cctatagcta ctacgagaag cttcacacct atttccctgt ctcctcactg ggggtgctgc 1200 aggaggactc gtccaacatc gtggagctgc tggaggaggc cttcaatcgg atccgctcca 1260 acctggacat ccgggcccta gacagccccc gaggccttcg gacagaggtc acctccaaga 1320 tgttccagaa gacgaggact gggtcctttc acatccggcg gggggaagtg ggtatatacc 1380 aggtgcagct gcgggccctt gagcacgtgg atgggacgca cgtgtgccag ctgccggagg 1440 accagaaggg caacatccat ctgaaacctt ccttctccga cggcctcaag atggacgcgg 1500 gcatcatctg tgatgtgtgc acctgcgagc tgcaaaaaga ggtgcggtca gctcgctgca 1560 gcttcaacgg agacttcgtg tgcggacagt gtgtgtgcag cgagggctgg agtggccaga 1620 cctgcaactg ctccaccggc tctctgagtg acattcagcc ctgcctgcgg gagggcgagg 1680 acaagccgtg ctccggccgt ggggagtgcc agtgcgggca ctgtgtgtgc tacggcgaag 1740 gccgctacga gggtcagttc tgcgagtatg acaacttcca gtgtccccgc acttccgggt 1800 tcctctgcaa tgaccgagga cgctgctcca tgggccagtg tgtgtgtgag cctggttgga 1860 caggcccaag ctgtgactgt cccctcagca atgccacctg catcgacagc aatgggggca 1920 tctgtaatgg acgtggccac tgtgagtgtg gccgctgcca ctgccaccag cagtcgctct 1980 acacggacac catctgcgag atcaactact cggcgatcca cccgggcctc tgcgaggacc 2040 tacgctcctg cgtgcagtgc caggcgtggg gcaccggcga gaagaagggg cgcacgtgtg 2100 aggaatgcaa cttcaaggtc aagatggtgg acgagcttaa gagagccgag gaggtggtgg 2160 tgcgctgctc cttccgggac gaggatgacg actgcaccta cagctacacc atggaaggtg 2220 acggcgcccc tgggcccaac agcactgtcc tggtgcacaa gaagaaggac tgccctccgg 2280 gctccttctg gtggctcatc cccctgctcc tcctcctcct gccgctcctg gccctgctac 2340 tgctgctatg ctggaagtac tgtgcctgct gcaaggcctg cctggcactt ctcccgtgct 2400 gcaaccgagg tcacatggtg ggctttaagg aagaccacta catgctgcgg gagaacctga 2460 tggcctctga ccacttggac acgcccatgc tgcgcagcgg gaacctcaag ggccgtgacg 2520 tggtccgctg gaaggtcacc aacaacatgc agcggcctgg ctttgccact catgccgcca 2580 gcatcaaccc cacagagctg gtgccctacg ggctgtcctt gcgcctggcc cgcctttgca 2640 ccgagaacct gctgaagcct gacactcggg agtgcgccca gctgcgccag gaggtggagg 2700 agaacctgaa cgaggtctac aggcagatct ccggtgtaca caagctccag cagaccaagt 2760 tccggcagca gcccaatgcc gggaaaaagc aagaccacac cattgtggac acagtgctga 2820 tggcgccccg ctcggccaag ccggccctgc tgaagcttac agagaagcag gtggaacaga 2880 gggccttcca cgacctcaag gtggcccccg gctactacac cctcactgca gaccaggacg 2940 cccggggcat ggtggagttc caggagggcg tggagctggt ggacgtacgg gtgcccctct 3000 ttatccggcc tgaggatgac gacgagaagc agctgctggt ggaggccatc gacgtgcccg 3060 caggcactgc caccctcggc cgccgcctgg taaacatcac catcatcaag gagcaagcca 3120 gagacgtggt gtcctttgag cagcctgagt tctcggtcag ccgcggggac caggtggccc 3180 gcatccctgt catccggcgt gtcctggacg gcgggaagtc ccaggtctcc taccgcacac 3240 aggatggcac cgcgcagggc aaccgggact acatccccgt ggagggtgag ctgctgttcc 3300 agcctgggga ggcctggaaa gagctgcagg tgaagctcct ggagctgcaa gaagttgact 3360 ccctcctgcg gggccgccag gtccgccgtt tccacgtcca gctcagcaac cctaagtttg 3420 gggcccacct gggccagccc cactccacca ccatcatcat cagggaccca gatgaactgg 3480 accggagctt cacgagtcag atgttgtcat cacagccacc ccctcacggc gacctgggcg 3540 ccccgcagaa ccccaatgct aaggccgctg ggtccaggaa gatccatttc aactggctgc 3600 ccccttctgg caagccaatg gggtacaggg taaagtactg gattcagggt gactccgaat 3660 ccgaagccca cctgctcgac agcaaggtgc cctcagtgga gctcaccaac ctgtacccgt 3720 attgcgacta tgagatgaag gtgtgcgcct acggggctca gggcgaggga ccctacagct 3780 ccctggtgtc ctgccgcacc caccaggaag tgcccagcga gccagggcgt ctggccttca 3840 atgtcgtctc ctccacggtg acccagctga gctgggctga gccggctgag accaacggtg 3900 agatcacagc ctacgaggtc tgctatggcc tggtcaacga tgacaaccga cctattgggc 3960 ccatgaagaa agtgctggtt gacaacccta agaaccggat gctgcttatt gagaaccttc 4020 gggagtccca gccctaccgc tacacggtga aggcgcgcaa cggggccggc tgggggcctg 4080 agcgggaggc catcatcaac ctggccaccc agcccaagag gcccatgtcc atccccatca 4140 tccctgacat ccctatcgtg gacgcccaga gcggggagga ctacgacagc ttccttatgt 4200 acagcgatga cgttctacgc tctccatcgg gcagccagag gcccagcgtc tccgatgaca 4260 ctgagcacct ggtgaatggc cggatggact ttgccttccc gggcagcacc aactccctgc 4320 acaggatgac cacgaccagt gctgctgcct atggcaccca cctgagccca cacgtgcccc 4380 accgcgtgct aagcacatcc tccaccctca cacgggacta caactcactg acccgctcag 4440 aacactcaca ctcgaccaca ctgccgaggg actactccac cctcacctcc gtctcctccc 4500 acgactctcg cctgactgct ggtgtgcccg acacgcccac ccgcctggtg ttctctgccc 4560 tggggcccac atctctcaga gtgagctggc aggagccgcg gtgcgagcgg ccgctgcagg 4620 gctacagtgt ggagtaccag ctgctgaacg gcggtgagct gcatcggctc aacatcccca 4680 accctgccca gacctcggtg gtggtggaag acctcctgcc caaccactcc tacgtgttcc 4740 gcgtgcgggc ccagagccag gaaggctggg gccgagagcg tgagggtgtc atcaccattg 4800 aatcccaggt gcacccgcag agcccactgt gtcccctgcc aggctccgcc ttcactttga 4860 gcactcccag tgccccaggc ccgctggtgt tcactgccct gagcccagac tcgctgcagc 4920 tgagctggga gcggccacgg aggcccaatg gggatatcgt cggctacctg gtgacctgtg 4980 agatggccca aggaggaggg ccagccaccg cattccgggt ggatggagac agccccgaga 5040 gccggctgac cgtgccgggc ctcagcgaga acgtgcccta caagttcaag gtgcaggcca 5100 ggaccactga gggcttcggg ccagagcgcg agggcatcat caccatagag tcccaggatg 5160 gaggaccctt cccgcagctg ggcagccgtg ccgggctctt ccagcacccg ctgcaaagcg 5220 agtacagcag catcaccacc acccacacca gcgccaccga gcccttccta gtggatgggc 5280 tgaccctggg ggcccagcac ctggaggcag gcggctccct cacccggcat gtgacccagg 5340 agtttgtgag ccggacactg accaccagcg gaacccttag cacccacatg gaccaacagt 5400 tcttccaaac ttgaccgcac cctgccccac ccccgccatg tcccactagg cgtcctcccg 5460 actcctctcc cggagcctcc tcagctactc catccttgca cccctggggg cccagcccac 5520 ccgcatgcac agagcagggg ctaggtgtct cctgggaggc atgaaggggg caaggtccgt 5580 cctctgtggg cccaaaccta tttgtaacca aagagctggg agcagcacaa ggacccagcc 5640 tttgttctgc acttaataaa tggttttgct actgctaaaa a 5681 59 1366 DNA Homo sapiens misc_feature Incyte ID No 1256295.18 59 ctttgtcctc cagtggctgg taggcagtgg ctgggaggca gcggcccaat tagtgtcgtg 60 cggcccgtgg cgaggcgagg tccggggagc gagcgagcaa gcaaggcggg aggggtggcc 120 ggagctgcgg cggctggcac aggaggagga gcccgggcgg gcgaggggcg gccggagagc 180 gccagggcct gagctgccgg agcggcgcct gtgagtgagt gcagaaagca ggcgcccgcg 240 cgctagccgt ggcaggagca gcccgcacgc cgcgctctct ccctgggcga cctgcagttt 300 gcaatatgac tttggaggaa ttctcggctg gagagcagaa gaccgaaagg atggataagg 360 tgggggatgc cctggaggaa gtgctcagca aagccctgag tcagcgcacg atcactgtcg 420 gggtgtacga agcggccaag ctgctcaacg tcgaccccga taacgtggtg ttgtgcctgc 480 tggcggcgga cgaggacgac gacagagatg tggctctgca gatccacttc accctgatcc 540 aggcgttttg ctgcgagaac gacatcaaca tcctgcgcgt cagcaacccg ggccggctgg 600 cggagctcct gctcttggag accgacgctg gccccgcggc gagcgagggc gccgagcagc 660 ccccggacct gcactgcgtg ctggtgacga atccacattc atctcaatgg aaggatcctg 720 ccttaagtca acttatttgt ttttgccggg aaagtcgcta catggatcaa tgggttccag 780 tgattaatct ccctgaacgg tgatggcatc tgaatgaaaa taactgaacc aaattgcact 840 gaagtttttg aaataccttt gtagttactc aagcagttac tccctacact gatgcaagga 900 ttacagaaac tgatgccaag gggctgagtg agttcaacta catgttctgg gggcccggag 960 atagatgact ttgcagatgg aaagaggtga aaatgaagaa ggaagctgtg ttgaaacaga 1020 aaaataagtc aaaaggaaca aaaattacaa agaaccatgc aggaaggaaa actatgtatt 1080 aatttagaat ggttgagtta cattaaaata aaccaaatat gttaaagttt aagtgtgcag 1140 ccatagtttg ggtatttttg gtttatatgc cctcaagtaa aagaaaagcc gaaagggtta 1200 atcatatttg aaaaccatat tttattgtat tttgatgaga tattaaattc tcaaagtttt 1260 attataaatt ctactaagtt attttatgac atgaaaagtt atttatgcta taaatttttt 1320 gaaacacaat acctacaata aactggtatg aataattgca tcattt 1366 60 1432 DNA Homo sapiens misc_feature Incyte ID No 444096.1 60 gacccatcag ggcttctgta aggctgagtg ggtcccatgc ctgaaaggag agccaggctg 60 agcctggcct gagtctccca tgtgtaacag gtacgaggat gaaatcaaca agcacactgc 120 tgcagagaac gagtttgtgg tgctcaagaa ggatgtggat gcagcataca tgggccggat 180 ggatctgcat ggcaaagtgg gcaccttgac ccaggagatt gacttcctgc agcaactcta 240 tgaaatggag ctgagccaag tgcagaccca cgtgtctaac accaatgtgg tgctgtccat 300 ggacaacaac cgcaacctgg acctggacag catcatcgcc gaggtcaagg cccagtatga 360 gctgattgcc cagaggagcc gggctgaggc cgaggcctgg taccagacca agtatgagga 420 gctgcaggtg actgctggga agcatgggga caacctgcgg gacaccaaga acgagattgc 480 tgagctcacc cgcactatcc agaggctgca gggggaggct gatgcagcca agaagcagtg 540 tcagcagctg cagacggcca ttgcggaacg cggagcagcg tggggagctg gcactcaagg 600 atgctcagaa gaagcttggg gatctggatg tggccctgca ccaggccaag gaggacctga 660 cacggctgct gcgtgactac caggagctga tgaatgtcaa gctggccctg gacgtggaga 720 ttgccaccta ccgcaagctt ctggagagcg aggagagcag gatgtctgga gaatgtccca 780 gtgcagtcag catttctgtg actggcaact ccaccactgt gtgcggaggt ggcgcaccag 840 ctttggaggt ggcatctccc tgggtgggag tgggggggcc accaagggtg gattcagcac 900 aaatgtgggc tatagcaccg tcaagggagg gccagtctct gcgggcacct ccatcctgcg 960 gaagaccact acggtcaaga cgtccagcca gaggtattag ctgctgagcc ctgcaaggcc 1020 ccctgcaatc atgtccctgc cctcctcacc ccacctctgc tgtcctttcc agtcacttct 1080 caggagcagg aacagccagg ggacctcaga cccagggtat tttcatacca gactatttgc 1140 atcttgggaa gcgctcaaat ctactcaggt tttctccttg gtcctgcagt aggatgggag 1200 ggaaggttaa agttgccagc ttgagtgatg tgcttgggtg acttgggggt gaccttttga 1260 ccaccgagag gaggctgaat ttctcaagcc attaggagag agagaaattg ggagtggtcc 1320 ccaaagaccc ttcaacctcc ccagtccccc accagaccca ccctctccct gaatctaccc 1380 acatccccct tccctgtctg tgtctcaata aatggtgcaa ctgcaaaaaa aa 1432 61 4559 DNA Homo sapiens misc_feature Incyte ID No 008942.10 61 agcgggcggc gcgcacactg ctcgctgggc cgcggctccc gggtgtccca ggcccggccg 60 gtgcgcagag catggcgggt gcgggcccga agcggcgcgc gctagcggcg ccggcggccg 120 aggagaagga agaggcgcgg gagaagatgc tggccgccaa gagcgcggac ggctcggcgc 180 cggcaggcga gggcgagggc gtgaccctgc agcggaacat cacgctgctc aacggcgtgg 240 ccatcatcgt ggggaccatt atcggctcgg gcatcttcgt gacgcccacg ggcgtgctca 300 aggaggcagg ctcgccgggg ctggcgctgg tggtgtgggc cgcgtgcggc gtcttctcca 360 tcgtgggcgc gctctgctac gcggagctcg gcaccaccat ctccaaatcg ggcggcgact 420 acgcctacat gctggaggtc tacggctcgc tgcccgcctt cctcaagctc tggatcgagc 480 tgctcatcat ccggccttca tcgcagtaca tcgtggccct ggtcttcgcc acctacctgc 540 tcaagccgct cttccccacc tgcccggtgc ccgaggaggc agccaagctc gtggcctgcc 600 tgtgcgtgct gctgctcacg gccgtgaact gctacagcgt gaaggccgcc acccgggtcc 660 aggatgcctt tgccgccgcc aagctcctgg ccctggccct gatcatcctg ctgggcttcg 720 tccagatcgg gaagggtgat gtgtccaatc tagatcccaa cttctcattt gaaggcacca 780 aactggatgt ggggaacatt gtgctggcat tatacagcgg cctctttgcc tatggaggat 840 ggaattactt gaatttcgtc acagaggaaa tgatcaaccc ctacagaaac ctgcccctgg 900 ccatcatcat ctccctgccc atcgtgacgc tggtgtacgt gctgaccaac ctggcctact 960 tcaccaccct gtccaccgag cagatgctgt cgtccgaggc cgtggccgtg gacttcggga 1020 actatcacct gggcgtcatg tcctggatca tccccgtctt cgtgggcctg tcctgctttg 1080 gctccgtcaa tgggtccctg ttcacatcct ccaggctctt cttcgtgggg tcccgggaag 1140 gccacctgcc ctccatcctc tccatgatcc acccacagct cctcaccccc gtgccgtccc 1200 tcgtgttcac gtgtgtgatg acgctgctct acgccttctc caaggacatc ttctccgtca 1260 tcaacttctt cagcttcttc aactggctct gcgtggccct ggccatcatc ggcatgatct 1320 ggctgcgcca cagaaagcct gagcttgagc ggcccatcaa ggtgaacctg gccctgcctg 1380 tgttcttcat cctggcctgc ctcttcctga tcgccgtctc cttctggaag acacccgtgg 1440 agtgtggcat cggcttcacc atcatcctca gcgggctgcc cgtctacttc ttcggggtct 1500 ggtggaaaaa caagcccaag tggctcctcc agggcatctt ctccacgacc gtcctgtgtc 1560 agaagctcat gcaggtggtc ccccaggaga catagccagg aggccgagtg gctgccggag 1620 gagcatgcgc agaggccagt taaagtagat cacctcctcg aacccactcc ggttccccgc 1680 aacccacagc tcagctgccc atcccagtcc ctcgccgtcc ctcccaggtc gggcagtgga 1740 ggctgctgtg aaaactctgg tacgaatctc atccctcaac tgagggccag ggacccaggt 1800 gtgcctgtgc tcctgcccag gagcagcttt tggtctcctt gggccctttt tcccttccct 1860 cctttgttta cttatatata tatttttttt aaacttaaat tttgggtcaa cttgacacca 1920 ctaagatgat tttttaagga gctgggggaa ggcaggagcc ttcctttctc ctgccccaag 1980 ggcccagacc ctgggcaaac agagctactg agacttggaa cctcattgct accacagact 2040 tgcactgaag ccggacagct gcccagacac atgggcttgt gacattcgtg aaaaccaacc 2100 ctgtgggctt atgtctctgc cttagggttt gcagagtgga aactcagccg tagggtggca 2160 ctgggagggg gtgggggatc tgggcaaggt gggtgattcc tcccaggagg tgcttgaggc 2220 cccgatggac tcctgaccat aatcctagcc ccgagacacc atcctgagcc agggaacagc 2280 cccagggttg gggggtgccg gcatctcccc tagctcacca ggcctggcct ctgggcagtg 2340 tggcctcttg gctatttctg tgtccagttt tggaggctga gttctggttc atgcagacaa 2400 agccctgtcc ttcagtcttc tagaaacaga gacaagaaag gcagacacac cgcggccagg 2460 cacccatgtg ggcgcccacc ctgggctcca cacagcagtg tcccctgccc cagaggtcgc 2520 agctaccctc agcctccaat gcattggcct ctgtaccgcc cggcagcccc ttctggccgg 2580 tgctgggttc ccactcccgg cctaggcacc tccccgctct ccctgtcacg ctcatgtcct 2640 gtcctggtcc tgatgcccgt tgtctaggag acagagccaa gcactgctca cgtctctgcc 2700 gcctgcgttt ggaggcccct gggctctcac ccagtcccca cccgcctgca gagagggaac 2760 tagggcaccc cttgtttctg ttgttcccgt gaattttttt cgctatggga ggcagccgag 2820 gcctggccaa tgcggcccac tttcctgagc tgtcgctgcc tccatggcag cagccaagga 2880 cccccagaac aagaagaccc ccccgcagga tccctcctga gctcgggggg ctctgccttc 2940 tcagggcccc gggcttccct tctccccagc cagaggtgga gccaagtggt ccagcgtcac 3000 tccagtgctc agctgtggct ggaggagctg gcctgtggca cagccctgag tgtcccaagc 3060 cgggagccaa cgaagccgga cacggcttca ctgaccagcg gctgctcaag ccgcaagctc 3120 tcagcaagtg cccagtggag cctgccgccc ccacctgggc accgggaccc cctcaccatc 3180 cagtgggccc ggagaaacct gatgaacagt ttggggactc aggaccagat gtccgtctct 3240 cttgcttgag gaatgaagac ctttattcac ccctgccccg ttgcttcccg ctgcacatgg 3300 acagacttca cagcgtctgc tcataggacc tgcatccttc ctggggacga attccactcg 3360 tccaagggac agcccacggt ctggaggccg aggaccacca gcaggcaggt ggactgactg 3420 ttgggcaaga cctcttccct ctgggcctgt tctcttggct gcaaataagg acagcagctg 3480 gtgccccacc tgcctggtgc attgctgtgt gaatccagga ggcagtggac atcgtaggca 3540 gccacggccc cgggtccagg agaagtgctc cctggaggca cgcaccactg cttcccactg 3600 gggccggcgg ggcccacgca cgacgtcagc ctcttacctt cccgcctcgg ctaggggtcc 3660 tcgggatgcc gttctgttcc aacctcctgc tctgggacgt ggacatgcct caaggataca 3720 gggagccggc ggcctctcga cggcacgcac ttgcctgttg gctgctgcgg ctgtgggcga 3780 gcatgggggc tgccagcgtc tgttgtggaa agtagctgct agtgaaatgg ctggggccgc 3840 tggggtccgt cttcacactg cgcaggtctc ttctgggcgt ctgagctggg gtgggagctc 3900 ctccgcagaa ggttggtggg gggtccagtc tgtgatcctt ggtgctgtgt gccccactcc 3960 agcctgggga ccccacttca gaaggtaggg gccgtgtccc gcggtgctga ctgaggcctg 4020 cttccccctc cccctcctgc tgtgctggaa ttccacaggg accagggcca ccgcagggga 4080 ctgtctcaga agacttgatt tttccgtccc tttttctcca cactccactg acaaacgtcc 4140 ccagcggttt ccacttgtgg gcttcaggtg ttttcaagca caacccacca caacaagcaa 4200 gtgcattttc agtcgttgtg cttttttgtt ttgtgctaac gtcttactaa tttaaagatg 4260 ctgtcggcac catgtttatt tatttccagt ggtcatgctc agccttgctg ctctgcgtgg 4320 cgcaggtgcc atgcctgctc cctgtctgtg tcccagccac gcagggccat ccactgtgac 4380 gtcggccgac caggctggac accctctgcc gagtaatgac gtgtgtggct gggaccttct 4440 ttattctgtg ttaatggcta acctgttaca ctgggctggg ttgggtaggg tgttctggct 4500 tttttgtggg gtttttattt ttaaagaaac actcaatcat cctaaaaaaa aattaaaaa 4559 62 1756 DNA Homo sapiens misc_feature Incyte ID No 008942.9 62 agtccccaca ccgcctgcag agagggaact agggcaccac cttgtttcat gttgttcccg 60 tgaatttttt tcagctatgg gaggcaaccg aggcactggc caaatgcagg cccaacattt 120 cactgagcat gtcagcatgc acatcacaat ggcaagcagc cagggaccca ccaagaacaa 180 gaagacccca gcaggatccc tcactgagca tcggggggca tctgcacttc atcaggcacc 240 ccagggcatt caccattcat cacaccaagc acagaggtgg agcacaagtg gtccagcgtc 300 acatccaagt gctcagctgt ggctggagga gctggcctgt ggcacagcca ctgagtgtcc 360 acaagccagg gagcacaacg atagccagga cacaggcttc actgaccagc aggctgcatc 420 aagccagcaa gcatctcagc aagtgcacca gtggagcact gccagcaccc cagcactggg 480 cacacaggga ccccacatca ccagtccagt gggccacgga gaaacactga tgcccgttgt 540 ctaggagaca gagcacaagc actgctcacg tctctgccgc ctgcgtttgg aggcccctgg 600 gctctcaccc agtccccacc cgcctgcaga gagggaacta gggcacccct tgtttctgtt 660 gttcccgtga atttttttcg ctatgggagg cagccgaggc ctggccaatg cggcccactt 720 tcctgagctg tcgctgcctc catggcagca gccagggacc cccagaacaa gaagaccccg 780 caggatccct cctgagctcg gggggctctg ccttctcagg ccccgggctt cccttctccc 840 cagccagagg tggagccaag tggtccagcg tcactccagt gctcagctgt ggctggagga 900 gctggcctgt ggcacagccc tgagtgtccc aagccgggag ccaacgaagc cggacacggc 960 ttcactgacc agcggctgct caagccgcaa gctctcagca agtgcccagt ggagcctgcc 1020 gcccccgcct gggcaccggg accccctcac catccagtgg gcccggagaa acctgatgaa 1080 cagtttgggg actcaggacc agatgtccgt ctctcttgct tgaggaatga agacctttat 1140 tcacccctgc cccgttgctt cccgctgcac atggacagac ttcacagcgt ctgctcatag 1200 gacctgcatc cttcctgggg acgaattcca ctcgtccaag ggacagccca cggtctggag 1260 gccgaggacc accagcaggc aggtggactg actgtgttgg gcaagacctc ttccctctgg 1320 gcctgttctc ttggctgcaa ataaggacag cagctggtgc cccacctgcc tggtgcattg 1380 ctgtgtgaat ccaggaggca gtggacatcg taggcagcca cggccccggg tccaggagaa 1440 gtgctccctg gaggcacgca ccactgcttc ccactggggc cggcggggcc cacgcacgac 1500 gtcagcctct taccttcccg cctcggctag gggtcctcgg gatgccgttc tgttccaacc 1560 tcctgctctg ggacgtggac atgcctcaac tgagggccag ggacccaggt gtgcctgtgc 1620 tcctgcccag gagcagcttt tggtctcctt gggccctttt tcccttccct cctttgttta 1680 cttatatata tatttttttt aaacttaaat tttgggtcaa cttgacacca ctaagatgat 1740 ttttaaggag ctgggg 1756 63 3304 DNA Homo sapiens misc_feature Incyte ID No 1252415.1 63 gcggaactct gaggtgaggg tgtgcagctt ggtagggatt ggggtccctt ccggggccca 60 tcggcccctg gtggtgttaa tggcccttct ggcctacgcg cgtgtcatga accctggccg 120 agagggccgg ggctgaggcc ctcaggccga cccggactct tgggcgcggt ctcttgaggt 180 ggggccgggg tgagcagctg agtccgggtg ccccggggag gcccctctgg cccgatttcg 240 cagcgctgcc catcagcttc agcggaggcc tgattcctga ggtgctctga ctggaaggaa 300 cctccgagat cggagagtct tccctgtctc ctgttgatgc tcccattgca ctgataggta 360 aattgatccc tagagaagag gctagtctga gatatatagc gagtgaggaa aagaatcgga 420 atcatgatcc tggtgcctta gataaccagc cccagttctt cccgtgttgc tcggaacctc 480 tctaacttgg gatggtcttc cggtcggtgt tgccccgcag gctgctgcag cttaaaggcc 540 agcgctgcgt ggaacttttt tttttctctc ctcccaaatt gagccgtttg aaatgcctag 600 ggagttttta aaagaaaggc gggcacatcc ttgtatttac aggcagatat cctccctttc 660 ctcctcggct gctgctctta ctttgacaag ccaggctaac attgaaggtg gtccattatg 720 gctgacatgc aaaatctggt agaaagattg gagagggcag tgggccgcct ggaggcagta 780 tctcatacct ctgacatgca ccgtgggtat gcagacagtc cttcaaaagc aggagcagct 840 ccatatgtgc aggcatttga ctcgctgctt gctggtcctg tggcagagta cttgaagatc 900 agtaaagaga ttgggggaga cgtgcagaaa catgcggaga tggtccacac aggtttgaag 960 ttggagcgag ctctgttggt tacagcttct cagtgtcaac agccagcaga aaataagctt 1020 tccgatttgt tggcacccat ctcagagcag atcaaagaag tgataacctt tcgggagaag 1080 aaccgaggca gcaagttgtt taatcacctg tcagctgtca gcgaaagtat ccaggccctg 1140 ggctgggtgg ctatggctcc caagcctggc ccttatgtga aagaaatgaa tgatgccgcc 1200 atgttttata caaaccgagt cctcaaagag tacaaagatg tggataagaa gcatgtagac 1260 tgggtcaaag cttatttaag tatatggaca gagctgcagg cttacattaa ggagttccat 1320 accaccggac tggcctggag caaaacgggg cctgtggcaa aagaactgag cggactgcca 1380 tctggaccct ctgccggatc aggtcctcct ccccctccac caggcccccc tcctccccca 1440 gtctctacca gttcaggctc agatgagtct gcttcccgct cagcactgtt cgcgcagatt 1500 aatcaggggg agagcattac acatgccctg aaacatgtat ctgatgacat gaagactcac 1560 aagaaccctg ccctgaaggc tcagagtggt ccagtacgca gtggccccaa accattctct 1620 gcacctaaac cccaaaccag cccatccccc aaacgagcca caaagaagga gccagctgta 1680 cttgaactgg agggcaagaa gtggagagtg gaaaatcagg aaaatgtttc caacctggtg 1740 attgaggaca cagagctgaa acaggtggct tacatataca agtgtgtcaa cacgacattg 1800 caaatcaagg gcaaaattaa ctccattaca gtagataact gtaagaaact tggcctggta 1860 ttcgatgacg tggtgggcat tgtggagata atcaacagta aggatgtcaa agttcaggta 1920 atgggtaaag tgccaaccat atccatcaac aaaacagatg gctgccatgc ttacctgagc 1980 aagaattccc tggattgtga aatagtcagt gccaaatctt ccgagatgaa tgtcctcatt 2040 cctacagaag gcggtgactt taatgaattc ccagttcctg agcagttcaa gaccctatgg 2100 aacgggcaga agttggtcac cacagtgaca gaaattgctg gataagcgaa gtgccactgg 2160 gttctttgcc ctcccttcac accatgggat aaatctgtat caagacggtt cttttctaga 2220 tttcctctac ctttttgctc ttaaaactgc ttctctgctc tgagaagcac agctacctgc 2280 cttcactgaa atatacctca ggctgaaatt tggggtggga tagcaggtca gttgatcttc 2340 tgcaggaagg tgcagctttt ccatatcagc tcaaccacgc cgccagtcca ttcttaagga 2400 actgccgact aggactgatg atgcatttta gctttgagct tttgggggtt attctaccaa 2460 caaacagtcc attggaaaga aaacagtccc tggaattaac agatcagaat gttcacactg 2520 gttaatcttt ttttaacaat gagcatgaag gtagcagaag ctggtgtgtt tccagatggt 2580 tcttctaacc aaactaattt ttcactgttg acaagcgagg caagggttgc actggaccaa 2640 aggctgaggc ttggccatct agcattccat acaaaattgt ttcctataag cattcctttt 2700 attctctatt ctatcctggg tctgcctcaa ccgtgagata ggagagtctc tggtactagc 2760 tgctgtagca gtgcccttca tccagggcag ttaatggagt cttggaccct ttctttctct 2820 gggatccctg cccagcacct tcctatagag atgactttaa aaggaaaaaa aaaaaaaaaa 2880 caaacccaca tgatttcaag gagtctggca ttcctgaatc cttcttccct gccaggtgcc 2940 tgtcacctgt cttcactgcc tccttttccc tgtcatgctc atcagcttat ggcttctgtc 3000 taagcacctg aacagaggac tgaaacctcc actgcaggct ggttttaggt cttgaattat 3060 gtaagaatct tgcacagcac tgctaatgta aatttcagtt gtttttccct ctaggacaaa 3120 cacttaccaa aatatgcaac ttttttttgg tgggaagaga gattgtcctg tgatttctac 3180 ccatttcctg aggcctgtgg aaataaacct ttatgtactt aaagttatac agaaaataga 3240 ataaagttaa taccaaactt gaaaaanaaa aaaaangggg ggccgccgnn tagtgancnc 3300 gtcg 3304 64 7231 DNA Homo sapiens misc_feature Incyte ID No 1399366.20 64 cccgagctgg cctgcgagtt cagggctcct gccgctctcc aggagcaacc tctactccgg 60 acgcacaggc attccccgcg cccctccagc cctcgccgcc ctcgccaccg ctcccggccg 120 ccgcgctccg gtacacacag gatccctgct gggcaccaac agctccacca tggggctggc 180 ctggggacta ggcgtcctgt tcctgatgca tgtgtgtggc accaaccgca ttccagagtc 240 tggcggagac aacagcgtgt ttgacatctt tgaactcacc ggggccgccc gcaaggggtc 300 tgggcgccga ctggtgaagg gccccgaccc ttccagccca gctttccgca tcgaggatgc 360 caacctgatc ccccctgtgc ctgatgacaa gttccaagac ctggtggatg ctgtgcgggc 420 agaaaagggt ttcctccttc tggcatccct gaggcagatg aagaagaccc ggggcacgct 480 gctggccctg gagcggaaag accactctgg ccaggtcttc agcgtggtgt ccaatggcaa 540 ggcgggcacc ctggacctca gcctgaccgt ccaaggaaag cagcacgtgg tgtctgtgga 600 agaagctctc ctggcaaccg gccagtggaa gagcatcacc ctgtttgtgc aggaagacag 660 ggcccagctg tacatcgact gtgaaaagat ggagaatgct gagttggacg tccccatcca 720 aagcgtcttc accagagacc tggccagcat cgccagactc cgcatcgcaa aggggggcgt 780 caatgacaat ttccaggggg tgctgcagaa tgtgaggttt gtctttggaa ccacaccaga 840 agacatcctc aggaacaaag gctgctccag ctctaccagt gtcctcctca cccttgacaa 900 caacgtggtg aatggttcca gccctgccat ccgcactaac tacattggcc acaagacaaa 960 ggacttgcaa gccatctgcg gcatctcctg tgatgagctg tccagcatgg tcctggaact 1020 caggggcctg cgcaccattg tgaccacgct gcaggacagc atccgcaaag tgactgaaga 1080 gaacaaagag ttggccaatg agctgaggcg gcctccccta tgctatcaca acggagttca 1140 gtacagaaat aacgaggaat ggactgttga tagctgcact gagtgtcact gtcagaactc 1200 agttaccatc tgcaaaaagg tgtcctgccc catcatgccc tgctccaatg ccacagttcc 1260 tgatggagaa tgctgtcctc gctgttggcc cagcgactct gcggacgatg gctggtctcc 1320 atggtccgag tggacctcct gttctacgag ctgtggcaat ggaattcagc agcgcggccg 1380 ctcctgcgat acgctcaaca accgatgtga gggctcctcg gtccagacac ggacctgcca 1440 cattcaggag tgtgacaaga gatttaaaca ggatggtggc tggagccact ggtccccgtg 1500 gtcatcttgt tctgtgacat gtggtgatgg tgtgatcaca aggatccggc tctgcaactc 1560 tcccagcccc cagatgaacg ggaaaccctg tgaaggcgaa gcgcgggaga ccaaagcctg 1620 caagaaagac gcctgcccca tcaatggagg ctggggtcct tggtcaccat gggacatctg 1680 ttctgtcacc tgtggaggag gggtacagaa acgtagtcgt ctctgcaaca accccacacc 1740 ccagtttgga ggcaaggact gcgttggtga tgtaacagaa aaccagatct gcaacaagca 1800 ggactgtcca attgatggat gcctgtccaa tccctgcttt gccggcgtga agtgtactag 1860 ctaccctgat ggcagctgga aatgtggtgc ttgtccccct ggttacagtg gaaatggcat 1920 ccagtgcaca gatgttgatg agtgcaaaga agtgcctgat gcctgcttca accacaatgg 1980 agagcaccgg tgtgagaaca cggaccccgg ctacaactgc ctgccctgcc ccccacgctt 2040 caccggctca cagcccttcg gccagggtgt cgaacatgcc acggccaaca aacaggtgtg 2100 caagccccgt aacccctgca cggatgggac ccacgactgc aacaagaacg ccaagtgcaa 2160 ctacctgggc cactatagcg accccatgta ccgctgcgag tgcaagcctg gctacgctgg 2220 caatggcatc atctgcgggg aggacacaga cctggatggc tggcccaatg agaacctggt 2280 gtgcgtggcc aatgcgactt accactgcaa aaaggataat tgccccaacc ttcccaactc 2340 agggcaggaa gactatgaca aggatggaat tggtgatgcc tgtgatgatg acgatgacaa 2400 tgataaaatt ccagatgaca gggacaactg tccattccat tacaacccag ctcagtatga 2460 ctatgacaga gatgatgtgg gagaccgctg tgacaactgt ccctacaacc acaacccaga 2520 tcaggcagac acagacaaca atggggaagg agacgcctgt gctgcagaca ttgatggaga 2580 cggtatcctc aatgaacggg acaactgcca gtacgtctac aatgtggacc agagagacac 2640 tgatatggat ggggttggag atcagtgtga caattgcccc ttggaacaca atccggatca 2700 gctggactct gactcagacc gcattggaga tacctgtgac aacaatcagg atattgatga 2760 agatggccac cagaacaatc tggacaactg tccctatgtg cccaatgcca accaggctga 2820 ccatgacaaa gatggcaagg gagatgcctg tgaccacgat gatgacaacg atggcattcc 2880 tgatgacaag gacaactgca gactcgtgcc caatcccgac cagaaggact ctgacggcga 2940 tggtcgaggt gatgcctgca aagatgattt tgaccatgac agtgtgccag acatcgatga 3000 catctgtcct gagaatgttg acatcagtga gaccgacttc cgccgattcc agatgattcc 3060 tctggacccc aaagggacat cccaaaatga ccctaactgg gttgtacgcc atcagggtaa 3120 agaactcgtc cagactgtca actgtgatcc tggactcgct gtaggttatg atgagtttaa 3180 tgctgtggac ttcagtggca ccttcttcat caacaccgaa agggacgatg actatgctgg 3240 atttgtcttt ggctaccagt ccagcagccg cttttatgtt gtgatgtgga agcaagtcac 3300 ccagtcctac tgggacacca accccacgag ggctcaggga tactcgggcc tttctgtgaa 3360 agttgtaaac tccaccacag ggcctggcga gcacctgcgg aacgccctgt ggcacacagg 3420 aaacacccct ggccaggtgc gcaccctgtg gcatgaccct cgtcacatag gctggaaaga 3480 tttcaccgcc tacagatggc gtctcagcca caggccaaag acgggtttca ttagagtggt 3540 gatgtatgaa gggaagaaaa tcatggctga ctcaggaccc atctatgata aaacctatgc 3600 tggtggtaga ctagggttgt ttgtcttctc tcaagaaatg gtgttcttct ctgacctgaa 3660 atacgaatgt agagatccct aatcatcaaa ttgttgattg aaagactgat cataaaccaa 3720 tgctggtatt gcaccttctg gaactatggg cttgagaaaa cccccaggat cacttctcct 3780 tggcttcctt cttttctgtg cttgcatcag tgtggactcc tagaacgtgc gacctgcctc 3840 aagaaaatgc agttttcaaa aacagactca gcattcagcc tccaatgaat aagacatctt 3900 ccaagcatat aaacaattgc tttggtttcc ttttgaaaaa gcatctactt gcttcagttg 3960 ggaaggtgcc cattccactc tgcctttgtc acagagcagg gtgctattgt gaggccatct 4020 ctgagcagtg gactcaaaag cattttcagg catgtcagag aagggaggac tcactagaat 4080 tagcaaacaa aaccaccctg acatcctcct tcaggaacac ggggagcaga ggccaaagca 4140 ctaaggggag ggcgcatacc cgagacgatt gtatgaagaa aatatggagg aactgttaca 4200 tgttcggtac taagtcattt tcaggggatt gaaagactat tgctggattt catgatgctg 4260 actggcgtta gctgattaac ccatgtaaat aggcacttaa atagaagcag gaaagggaga 4320 caaagactgg cttctggact tcctccctga tccccaccct tactcatcac ctgcagtggc 4380 cagaattagg gaatcagaat caaaccagtg taaggcagtg ctggctgcca ttgcctggtc 4440 acattgaaat tggtggcttc attctagatg tagcttgtgc agatgtagca ggaaaatagg 4500 aaaacctacc atctcagtga gcaccagctg cctcccaaag gaggggcagc cgtgcttata 4560 tttttatggt tacaatggca caaaattatt atcaacctaa ctaaaacatt ccttttctct 4620 tttttcctga attatcatgg agttttctaa ttctctcttt tggaatgtag atttttttta 4680 aatgctttac gatgtaaaat atttattttt tacttattct ggaagatctg gctgaaggat 4740 tattcatgga acaggaagaa gcgtaaagac tatccatgtc atctttgttg agagtcttcg 4800 tgactgtaag attgtaaata cagattattt attaactctg ttctgcctgg aaatttaggc 4860 ttcatacgga aagtgtttga gagcaagtag ttgacattta tcagcaaatc tcttgcaaga 4920 acagcacaag gaaaatcagt ctaataagct gctctgcccc ttgtgctcag agtggatgtt 4980 atgggattct ttttttctct gttttatctt ttcaagtgga attagttggt tatccatttg 5040 caaatgtttt aaattgcaaa gaaagccatg aggtcttcaa tactgtttta ccccatccct 5100 tgtgcatatt tccagggaga aggaaagcat atacactttt ttctttcatt tttccaaaag 5160 agaaaaaaat gacaaaaggt gaaacttaca tacaaatatt acctcatttg ttgtgtgact 5220 gagtaaagaa tttttggatc aagcggaaag agtttaagtg tctaacaaac ttaaagctac 5280 tgtagtacct aaaaagtcag tgttgtacat agcataaaaa ctctgcagag aagtattccc 5340 aataaggaaa tagcattgaa atgttaaata caatttctga aagttatgtt ttttatctat 5400 catctggtat accattgctt tatttttata aattattttc tcattgccat tggaatagat 5460 atctcagatt gtgtagatat gctatttaaa taatttatca ggaaatactg cctgtagagt 5520 tagtatttct atttttatat aatgtttgca cactgaattg aagaattgtt ggttttttct 5580 tttttttgtt ttgttttttt ntttttttnt ttttgctttt gacctcccat ttttactatt 5640 tgccaatacc tttttctagg aatgtgcttt tttttgtaca catttttatc cattttacat 5700 tctaaagcag tgtaagttgt atattactgt ttcttatgta caaggaacaa caataaatca 5760 tatggaaatt tatatttata cttactgtat ccatgcttat ttgttctcta ctggctttat 5820 gtcatgaagt atatgcgtaa ataccattca taaatcaata tagcatatac aaaaataaat 5880 tacagtaagt catagcaaca ttcacagttt gtatgtgatt gagaaagact gagttgctca 5940 ggcctaggct tagaatttgc tgcgtttgtg gaataaaaga acaaaatgat acattagcct 6000 gccatatcaa aaacatataa aagagaaatt atccctaagt caagggcccc cataagaata 6060 aaatttctta ttaaggtcat tagatgtcat tgaatccttt tcaaagtgca gtatgaaaac 6120 aaagggaaaa acactgaagc acacgcaact ctcacagcga cattttctga cccacgaatg 6180 atgccttggg tgggcaacac gattgcatgt tgtggagaca cttcggaagt aaatgtggat 6240 gagggaggag ctgtccttgc aatgttgagc caagcattac agatacctcc tcttgaagaa 6300 ggaataataa gtttaatcaa aaaagaagac taaaaaatgt aaaatttgga aggaatccat 6360 aaatgcgtgt gtgtctaaat acaaattatc atgtgaagaa aaggcccaag tgtaccaata 6420 agcagacctt gatttttgga tgggctaatt atgaatgtgg aatactgacc agttaatttc 6480 cagttttaat gaaaacagat caaagaagaa attttatgag taggttaaag gtctggcttt 6540 gaggtctatt aaacactaga aaggactggc tgggtgagat aaaatcttcc ttgttgattt 6600 tcactctcat tctataaata ctcatctttc tgagtagcca tgatcacata caaatgtaaa 6660 ttgccaaatc attttatagt accaaggtga agaagcagga actagaaagt gttgataata 6720 gctgtggagt taggaaaact gatgtgaagg aaataattct ttgaaatggc aaagaattaa 6780 ataccatcat tcattatcag aagagttcaa cgtttgaagt gctgggagat aattctaatt 6840 cattcttgga tagtgaagca aaactgattg aaaataccaa gataagacag aaaaagtgac 6900 tggaaagagg agcttttctt ccaggcatgt tccagtttca ccctaagact gaccttcaaa 6960 taatcaggtt gtactgaaat aaaggacttg ttaaaaatta aaattatgtc atcgagatga 7020 tagctttttt cctcctccaa cagtttattg tgcatgtgtt gtgggagagc tcgagtgaag 7080 agcaataaac tccaggtctt ataagantgt acatacaata aaggtggtgc cagcagtttt 7140 tttttttcta aagagtcaca tgtagaaaag cctccagtat taagctcctg aattcattcc 7200 tataaataaa ttggctctct ctctcttcta t 7231 65 961 DNA Homo sapiens misc_feature Incyte ID No 3732868CB1 65 ctggctctga ccgcgctgnc ctgggcccga gagcccagga ggcgtgtctc agagaaaaga 60 tataagcggc ccccggacgc taaagcggtg ccagcggcgg agtctccaac tgggagagct 120 gcagctgccg agaggaggag aacgctgagg tcggtcggac caacggacgc gctgaccgct 180 gccaactgca gctcgcgctg cctcctgctc gcgccgtgcc actaaggtca ctcccgcctc 240 cgagagccca gagccgagat ggaaacggtc caggagctga tccccctggc caaggagatg 300 atggcccaga agcgcaaggg gaagatggtg aagctgtacg tgctgggcag cgtgctggcc 360 ctcttcggcg tggtgctcgg cctgatggag actgtgtgca gccccttcac ggccgccaga 420 cgtctgcggg accaggaggc agccgtggcg gagctgcagg ccgccctgga gcgacaggct 480 ctccagaagc aagccctgca ggagaaaggc aagcagcagg acacggtcct cggcggccgg 540 gccctgtcca accggcagca cgcctcctag gaactgtggg agaccagcgg agtgggaggg 600 agacgcagta gacagagaca gaccgagaag gaagggagag acagaggggg cgcgcgcaca 660 ggagcctgac tccgctggga gagtgcagga gcacgtgctg ttttttattt ggacttaact 720 tcagagaaac cgctgacatc tagaactgac ctaccacaag catccaccaa aggagtttgg 780 gattgagttt tgctgctgtg cagcactgca ttgtcatgac atttccaaca ctgtgtgaat 840 tatctaaatg cgtctaccat tttgcactag ggaggaagga taaatgcttt ttatgttatt 900 attattaatt attacaatga ccaccatttt gcattttgaa ataaaaaact ttttatacca 960 t 961 66 103 PRT Homo sapiens misc_feature Incyte ID No 3732868CD1 66 Met Glu Thr Val Gln Glu Leu Ile Pro Leu Ala Lys Glu Met Met 1 5 10 15 Ala Gln Lys Arg Lys Gly Lys Met Val Lys Leu Tyr Val Leu Gly 20 25 30 Ser Val Leu Ala Leu Phe Gly Val Val Leu Gly Leu Met Glu Thr 35 40 45 Val Cys Ser Pro Phe Thr Ala Ala Arg Arg Leu Arg Asp Gln Glu 50 55 60 Ala Ala Val Ala Glu Leu Gln Ala Ala Leu Glu Arg Gln Ala Leu 65 70 75 Gln Lys Gln Ala Leu Gln Glu Lys Gly Lys Gln Gln Asp Thr Val 80 85 90 Leu Gly Gly Arg Ala Leu Ser Asn Arg Gln His Ala Ser 95 100 67 2608 DNA Homo sapiens misc_feature Incyte ID No 1137894.1 67 ttcagcgctc ccactctcgg ccgacacccc tgcatggcca accgttacac catggatctg 60 actgccatct acgaggtgag tccccgccgc acggcatccc cggtacctgc atgcctgagt 120 ccgagtcccc acctctctag cgccgcaaac tccagcccgg gacgcttgcc tcccttctcc 180 aactggggct ccctagcgcc gcgccctcca gcctggggcc cctgcctccc gctcagacca 240 gcttggtgat ttggaggtga aaatggaacc cgcgacaccc ggctcttcgc tcaaacatgg 300 gtggggcggc ccatgcaagt ggaaagtcgg agaacttttc tcagaccgag gctgcctgga 360 ggcggaagtg gcccccatac ctggctcacc cctagtcgtt gctgagggcg tggttttgcg 420 cggaggcgtc tctggggctg aagtctcagg gtggggggat ccgacttctg tctctccagt 480 ccctgaccgt agagacagag aaccctaaaa ccgaagcaat ccggacttcc aggtcaactt 540 tgcccggttt ctccagttgt gaaactggag atcccgacgc gtgggtcata tccggggagg 600 acaagagacc caaaattggg aaacagtggt gcgccctgac ttcggggtcc ccctcttggt 660 ccagccgggg aagccgggat tcctgggtcc ctcgggataa ggcctcggtg gtgggtaaac 720 tcagaacctc caactctggg ttcctggcat ccggaaccca ggggtttctg cgggcgggtg 780 gggctcaggc ggggagccca caaaccggcc tggcaagctc tagttccctg cagctggggt 840 ggggcgtcgc cctgcatttt caggtgcctt aaccgaccca tttccgcaga gcctcctgtc 900 gctgagccct gacgtgcccg tgccatccga ccatggaggg actgagtcca gcccaggctg 960 gggctcctcg ggaccctgga gcctgagccc ctccgactcc agcccgtctg gggtcacctc 1020 ccgcctgcct ggccgctcca ccagcctagt ggagggccgc agctgtggct gggtgccccc 1080 accccctggc ttcgcaccgc tggctccccg cctgggccct gagctgtcac cctcacccac 1140 ttcgcccact gcaacctcca ccaccccctc gcgctacaag actgagctat gtcggacctt 1200 ctcagagagt gggcgctgcc gctacggggc caagtgccag tttgcccatg gcctgggcga 1260 gctgcgccag gccaatcgcc accccaaata caagacggaa ctctgtcaca agttctacct 1320 ccagggccgc tgcccctacg gctctcgctg ccacttcatc cacaacccta gcgaagacct 1380 ggcggccccg ggccaccctc ctgtgcttcg ccagagcatc agcttctccg gcctgccctc 1440 tggccgccgg acctcaccac caccaccagg cctggccggc ccttccctgt cctccagctc 1500 cttctcgccc tccagctccc caccaccacc tggggacctt ccactgtcac cctctgcctt 1560 ctctgctgcc cctggcaccc ccctggctcg aagagacccc accccagtct gttgcccctc 1620 ctgccgaagg gccactccta tcagcgtctg ggggcccttg ggtggcctgg ttcggacccc 1680 ctctgtacag tccctgggat ccgaccctga tgaatatgcc agcagcggca gcagcctggg 1740 gggctctgac tctcccgtct tcgaggcggg agtttttgca ccaccccagc ccgtggcagc 1800 cccccggcga ctccccatct tcaatcgcat ctctgtttct gagtgacaaa gtgactgccc 1860 ggtcagatca gctggatctc agcggggagc cacgtctctt gcactgtggt ctctgcatgg 1920 accccagggc tgtggggact tgggggacag taatcaagta atcccctttt ccagaatgca 1980 ttaacccact cccctgacct cacgctgggg caggtcccca agtgtgcaag ctcagtattc 2040 atgatggtgg gggatggagt gtcttccgag gttcttgggg gaaaaaaaat tgtagcatat 2100 ttaagggagg caatgaaccc tctcccccac ctcttccctg cccaaatctg tctcctagaa 2160 tcttatgtgc tgtgaataat aggccttcac tgcccctcca gtttttatag acctgaggtt 2220 ccagtgtctc ctggtaactg gaacctctcc tgagggggaa tcctggtgct caaattaccc 2280 tccaaaagca agtagccaaa gccgttgcca aaccccaccc ataaatcaat gggcccttta 2340 tttatgacga ctttatttat tctaatatga ttttatagta tttatatata ttgggtcgtc 2400 tgcttccctt gtatttttct tccttttttt gtaatattga aaacgacgat ataattatta 2460 taagtagact ataatatatt tagtaatata tattattacc ttaaaagtct atttttgtgt 2520 tttgggcatt tttaaataaa caatctgagt gtgttcttcg tagaggaact cgattgagga 2580 ccagaggtcc tggacctcca aatacaac 2608 68 1527 DNA Homo sapiens misc_feature Incyte ID No 1418671CB1 68 gcttcctggg cgccgtgggc gcggactgcg cgggctgcgc gggtgccgag gagcgcgagg 60 cgcggggaag gcgcacctgg ggtggccctg gcgtgcgggc ggcgacatgg aggacggcgt 120 gctcaaggag ggcttcctgg tcaagagggg ccacattgtc cacaactgga aggcgcgatg 180 gttcatcctt cggcagaaca cgctggtgta ctacaagctt gaggggggtc ggagagtgac 240 ccctcccaag ggccggatcc tcctggatgg ctgcaccatc acctgcccct gcctggagta 300 tgaaaaccga ccgctcctca ttaagctgaa gactcaaaca tccacggagt acttcctgga 360 ggcctgttct cgagaggagc gggatgcctg ggcctttgag atcaccgggg ctattcatgc 420 agggcagccg gggaaggtcc agcagctgca cagcctgaga aactccttca agctgccccc 480 gcacatcagc ctgcatcgca ttgtggacaa gatgcacgat agcaacaccg gaatccgttc 540 aagccccaac atggagcagg gaagcaccta taaaaagacc ttcctcggct cctccctggt 600 ggactggctc atctccaaca gcttcacggc cagccgtctg gaggcggtga ccctggcctc 660 catgctcatg gaggagaact tcctcaggcc tgtgggtgtc cgaagcatgg gagccattcg 720 ctctggggat ctggccgagc agttcctgga tgactccaca gccctgtaca cttttgctga 780 gagctacaaa aagaagataa gccccaagga agaaattagc ctgagcactg tggagttaag 840 tggcacggtg gtgaaacaag gctacctggc caagcaggga cacaagagga aaaactggaa 900 ggtgcgtcgc tttgttctaa ggaaggatcc agctttcctg cattactatg acccttccaa 960 agaagagaac aggccagtgg gtgggttttc tcttcgtggt tcactcgtgt ctgctctgga 1020 agataatggc gttcccactg gggttaaagg gaatgtccag ggaaacctct tcaaagtgat 1080 tactaaggat gacacacact attacattca ggccagcagc aaggctgagc gagccgagtg 1140 gattgaagct atcaaaaagc taacatgaca aggacctgag ggaaccagga ttcctccctc 1200 ctaccagatg acacagacaa gagttcctgg agaatgggag tgttaagact tttgacttct 1260 ttgtaagttt tgtactgctt tggagagtga atgctgccaa gagttcctca gattacaaac 1320 agcagtggtg ccatttcctt ccccatcttc atgttacaaa cctggaaagg ctagaacagc 1380 cattaggcgt cagcatcttg acttttcccc agcatcacaa acagccattt cctcgggcac 1440 caaagtaggt tccctttgtt ggaacaatta cactggccat gccataatgt tgaataaaac 1500 tctcttctta tgaaaaaaaa aaaaaaa 1527 69 353 PRT Homo sapiens misc_feature Incyte ID No 1418671CD1 69 Met Glu Asp Gly Val Leu Lys Glu Gly Phe Leu Val Lys Arg Gly 1 5 10 15 His Ile Val His Asn Trp Lys Ala Arg Trp Phe Ile Leu Arg Gln 20 25 30 Asn Thr Leu Val Tyr Tyr Lys Leu Glu Gly Gly Arg Arg Val Thr 35 40 45 Pro Pro Lys Gly Arg Ile Leu Leu Asp Gly Cys Thr Ile Thr Cys 50 55 60 Pro Cys Leu Glu Tyr Glu Asn Arg Pro Leu Leu Ile Lys Leu Lys 65 70 75 Thr Gln Thr Ser Thr Glu Tyr Phe Leu Glu Ala Cys Ser Arg Glu 80 85 90 Glu Arg Asp Ala Trp Ala Phe Glu Ile Thr Gly Ala Ile His Ala 95 100 105 Gly Gln Pro Gly Lys Val Gln Gln Leu His Ser Leu Arg Asn Ser 110 115 120 Phe Lys Leu Pro Pro His Ile Ser Leu His Arg Ile Val Asp Lys 125 130 135 Met His Asp Ser Asn Thr Gly Ile Arg Ser Ser Pro Asn Met Glu 140 145 150 Gln Gly Ser Thr Tyr Lys Lys Thr Phe Leu Gly Ser Ser Leu Val 155 160 165 Asp Trp Leu Ile Ser Asn Ser Phe Thr Ala Ser Arg Leu Glu Ala 170 175 180 Val Thr Leu Ala Ser Met Leu Met Glu Glu Asn Phe Leu Arg Pro 185 190 195 Val Gly Val Arg Ser Met Gly Ala Ile Arg Ser Gly Asp Leu Ala 200 205 210 Glu Gln Phe Leu Asp Asp Ser Thr Ala Leu Tyr Thr Phe Ala Glu 215 220 225 Ser Tyr Lys Lys Lys Ile Ser Pro Lys Glu Glu Ile Ser Leu Ser 230 235 240 Thr Val Glu Leu Ser Gly Thr Val Val Lys Gln Gly Tyr Leu Ala 245 250 255 Lys Gln Gly His Lys Arg Lys Asn Trp Lys Val Arg Arg Phe Val 260 265 270 Leu Arg Lys Asp Pro Ala Phe Leu His Tyr Tyr Asp Pro Ser Lys 275 280 285 Glu Glu Asn Arg Pro Val Gly Gly Phe Ser Leu Arg Gly Ser Leu 290 295 300 Val Ser Ala Leu Glu Asp Asn Gly Val Pro Thr Gly Val Lys Gly 305 310 315 Asn Val Gln Gly Asn Leu Phe Lys Val Ile Thr Lys Asp Asp Thr 320 325 330 His Tyr Tyr Ile Gln Ala Ser Ser Lys Ala Glu Arg Ala Glu Trp 335 340 345 Ile Glu Ala Ile Lys Lys Leu Thr 350 70 5648 DNA Homo sapiens misc_feature Incyte ID No 464689.64 70 ggtgtggtgt cggtgtcggc agcatccccg gcgccctgct gcggtcgccg cgagcctcgg 60 cctctgtctc ctccccctcc cgcccttacc tccacgcggg accgcccgcg ccagtcaact 120 cctcgcactt tgcccctgct tggcagcgga taaaaggggg ctgaggaaat accggacacg 180 gtcacccgtt gccagctcta gcctttaaat tcccggctcg gggacctcca cgcaccgcgg 240 ctagcgccga caaccagcta gcgtgcaagg cgccgcggct cagcgcgtac cggcgggctt 300 cgaaaccgca gtcctccggc gaccccgaac tccgctccgg agcctcagcc ccctggaaag 360 tgatcccggc atcggagagc caagatgccg gcccacttgc tgcaggacga tatctctagc 420 tcctatacca ccaccaccac cattacagcg cctccctcca ggggtcctgc agaatggagg 480 agataagttg gagacgatgc ccctctactt ggaagacgac attcgccctg atataaaaga 540 tgatatatat gaccccacct acaaggataa ggaaggccca agccccaagg ttgaatatgt 600 ctggagaaac atcatcctta tgtctctgct acacttggga gccctgtatg ggatcacttt 660 gattcctacc tgcaagttct acacctggct ttggggggta ttctactatt ttgtcagtgc 720 cctgggcata acagcaggag ctcatcgtct gtggagccac cgctcttaca aagctcggct 780 gcccctacgg ctctttctga tcattgccaa cacaatggca ttccagaatg atgtctatga 840 atgggctcgt gaccaccgtg cccaccacaa gttttcagaa acacatgctg atcctcataa 900 ttcccgacgt ggctttttct tctctcacgt gggttggctg cttgtgcgca aacacccagc 960 tgtcaaagag aaggggagta cgctagactt gtctgaccta gaagctgaga aactggtgat 1020 gttccagagg aggtactaca aacctggctt gctgatgatg tgcttcatcc tgcccacgct 1080 tgtgccctgg tatttctggg gtgaaacttt tcaaaacagt gtgttcgttg ccactttctt 1140 gcgatatgct gtggtgctta atgccacctg gctggtgaac agtgctgccc acctcttcgg 1200 atatcgtcct tatgacaaga acattagccc ccgggagaat atcctggttt cacttggagc 1260 tgtgggtgag ggcttccaca actaccacca ctcctttccc tatgactact ctgccagtga 1320 gtaccgctgg cacatcaact tcaccacatt cttcattgat tgcatggccg ccctcggtct 1380 ggcctatgac cggaagaaag tctccaaggc cgccatcttg gccaggatta aaagaaccgg 1440 agatggaaac tacaagagtg gctgagtttg gggtccctca ggttcctttt tcaaaaacca 1500 gccaggcaga ggttttaatg tctgtttatt aactactgaa taatgctacc aggatgctaa 1560 agatgatgat gttaacccat tccagtacag tattctttta aaattcaaaa gtattgaaag 1620 ccaacaactc tgcctttatg atgctaagct gatattattt cttctcttat cctctctctc 1680 ttctaggccc attgtcctcc ttttcacttt attgctatcg ccctcctttc ccttattgcc 1740 tcccaggcaa gcagctggtc agtctttgct cagtgtccag cttccaaagc ctagacaacc 1800 tttctgtagc ctaaaacgaa tggtctttgc tccagataac tctctttcct tgagctgttg 1860 tgagctttga agtaggtggc ttgagctaga gataaaacag aatcttctgg gtagtcccct 1920 gttgattatc ttcagcccag gcttttgcta gatggaatgg aaaagcaact tcatttgaca 1980 caaagcttct aaagcaggta aattgtcggg ggagagagtt agcatgtatg aatgtaagga 2040 tgagggaagc gaagcaagag gaacctctcg ccatgatcag acatacagct gcctacctaa 2100 tgaggacttc aagccccacc acatagcatg cttcctttct ctcctggctc ggggtaaaaa 2160 gtggctgcgg tgtttggcaa tgctaattca atgccgcaac atatagttga ggccgaggat 2220 aaagaaagac attttaagtt tgtagtaaaa gtggtctctg ctggggaagg gtttcttttc 2280 ttttttcttt atcacaagga gatttcttag ttcatatatc aagaagtctt gaagttgggt 2340 gtttccagaa ttggtaaaaa cagcagctca tggaattttg agtattccat gagctgctca 2400 ttacagttct ttcctctttc tgctctgcca tcttcaggat attggttctt cccctcatag 2460 taataagatg gctgtggcat ttccaaacat ccaaaaaaag ggaaggattt aaggaggtga 2520 agtcgggtca aaaataaaat atatatacat atatacattg cttagaacgt taaactatta 2580 gagtatttcc cttccaaaga gggatgtttg gaaaaaactc tgaaggagag gaggaattag 2640 ttgggatgcc aatttcctct ccactgctgg acatgagatg gagaggctga gggacaggat 2700 ctataggcag cttctaagag cgaacttcac ataggaaggg atctgagaac acgttgccag 2760 gggcttgaga aggttactga gtgagttatt gggagtctta ataaaataaa ctagatatta 2820 ggtccattca ttaattagtt ccagtttctc cttgaaatga gtaaaaacta gaaggcttct 2880 ctccacagtg ttgtgcccct tcactcattt ttttttgagg agaagggggt ctctgttaac 2940 atctagccta aagtatacaa ctgcctgggg ggcagggtta ggaatctctt cactaccctg 3000 attcttgatt cctggctcta ccctgtctgt cccttttctt tgaccagatc tttctcttcc 3060 ctgaacgttt tcttctttcc ctggacaggc agcctccttt gtgtgtattc agaggcagtg 3120 atgacttgct gtccaggcag ctccctcctg cacacagaat gctcagggtc actgaaccac 3180 tgcttctctt ttgaaagtag agctagctgc cactttcacg tggcctccgc agtgtctcca 3240 cctacacccc tgtgctcccc tgccacactg atggctcaag acaaggctgg caaaccctcc 3300 cagaaacatc tctggcccag aaagcctctc tctccctccc tctctcatga ggcacagcca 3360 agccaagcgc tcatgttgag ccagtgggcc agccacagag caaaagaggg tttattttca 3420 gtcccctctc tctgggtcag aaccagaggg catgctgaat gccccctgct tacttggtga 3480 gggtgccccg cctgagtcag tgctctcagc tggcagtgca atgcttgtag aagtaggagg 3540 aaacagttct cactgggaag aagcaagggc aagaacccaa gtgcctcacc tcgaaaggag 3600 gccctgttcc ctggagtcag ggtgaactgc aaagctttgg ctgagacctg ggatttgaga 3660 taccacaaac cctgctgaac acagtgtctg ttcagcaaac taaccagcat tccctacagc 3720 ctagggcaga caatagtata gaagtctgga aaaaaacaaa aacagaattt gagaaccttg 3780 gaccactcct tgtccctgta gctcagtcat caaagcagaa gtcctggctt tgctctataa 3840 agaattggaa atggtacact acccaaacac tcagttcact tgttgagccc cagtgcctgg 3900 aagggaggaa ggcctttctt ctgtgttaat tgccgtagag gctacagggg ttagccctgg 3960 actaaaggca tccttgtctt ttgagctatt cacctcagta gaaaaggatc taagggaaga 4020 tcactgtagt ttagttctgt tgaccttgtg cacctacccc ttggaaatgt ctgctggtat 4080 ttctaattcc acaggtcatc agatgcctgc ttgataatat ataaacaata aaaacaactt 4140 tcacttcttc ctattgtaat cgtgtgccat ggatctgatc tgtaccatga ccctacataa 4200 ggctggatgg cacctcaggc tgagggcccc aatgtatgtg tggctgtggg tgtgggtggg 4260 agtgtgtctg ctgagtaagg aacacgattt tcaagattct aaagctcaat tcaagtgaca 4320 cattaatgat aaactcagat ctgatcaaga gtccggattt ctaacagtcc ttgctttggg 4380 ggggtgtgct gacaacttag ctcaggtgcc ttacatcttt tctaatcaca gtgttgcata 4440 tgagcctgcc ctcactccct ctgcagaatc cctttgcacc tgagacccta ctgaagtggc 4500 tggtagaaaa aggggcctga gtggaggatt atcagtatca cgatttgcag gattcccttc 4560 tgggcttcat tctggaaact tttgttaggg ctgcttttct taagtgccca catttgatgg 4620 agggtggaaa taatttgaat gtatttgatt tataagtttt tttttttttt ttgggttaaa 4680 agatggttgt agcatttaaa atggaaaatt ttctccttgg tttgctagta tcttgggtgt 4740 attctctgta agtgtagctc aaataggtca tcatgaaagg ttaaaaaagc gaggtggcca 4800 tgttatgctg gtggttaagg ccagggcctc tccaaccact gtgccactga cttgctgtgt 4860 gacctctggg caagtcactt aacgtataag gtgcctcagt tttccttctg ttaaaatggg 4920 gataataata ctgacctacc tcaaagggca gttttgaggc atgactaatg ctttttagaa 4980 agcattttgg gatccttcag cacaggaatt ctcaagacct gagtattttt tataatagga 5040 atgtccacca tgaacttgat acgtccgtgt gtcccagatg ctgtcattag tctatatggt 5100 tctccaagaa actgaatgaa tccattggag aagcggtgga taactagcca gacaaaattt 5160 gagaatacat aaacaacgca ttgccacgga aacatacaga ggatgccttt tctgtgattg 5220 ggtgggattt ttttcccttt ttatgtggga tatagtagtt acttgtgaca agaataattt 5280 tggaataatt tctattaata tcaactctga agctaattgt actaatctga gattgtggtg 5340 agcagtgacg atgaggagtt gtccagggac agagacgtat atgtgactac ccatactccc 5400 agaaacgcca gggatgaggg cgctacaggc ctcaggccct caggtactgt cagttgtccc 5460 atctgcatgg actggatact cagaggtaag taaaccaagc tgtatcttcc aggcttctgg 5520 tttctaaact tcactgaaag aattggatga gacaggatct tccccctcgg tgggattgga 5580 cacccctact cacagtcatg cctgggccct cacttattgc agatctgcct gtgaggggag 5640 aatgtgcc 5648 71 56 DNA Homo sapiens misc_feature Incyte ID No 053959.1 71 gngaggcaat ganccctctn ccccacctct tncctgccca natctgnctc ctagaa 56 72 580 DNA Homo sapiens misc_feature Incyte ID No 1384594.1 72 cttgggtgat ggggcacgga agagggttac aggcaaaggg accagcgttt ctaaactctt 60 ggagacacag tgaagaaggt tcatacctgg agtgccaagg ttactgtgtc tccagaaaca 120 catatggacc tcacaaagga cgagtgggga cttcttgatg aggctcagag actcctgtac 180 cttgaagtga tgctggagaa ctttgccctt gtagcctcac tgggttgtgg ccatggaaca 240 gaggatgaag agacaccttc tgaccagaat gtttactcta ggagtgtcac agtcaaaagg 300 caggttcatc caaaacagga gactccagtc ctgtggaaag tgtgtccaag tcctaaagat 360 aattttggat ctagctgaat ctcctagggc aggaaacata cttgggttcg ggagatgtac 420 aaacctggca caaggacaag aaggcttaac agtgcaaaga aaaaccttga taaggggcaa 480 tggacagagc ctcaaaaatg tggaagtgag gaccctagca tgtaagtcga tggaagccct 540 ttcgggaatt gggagggttt ggaaagggac cctccagacc 580 73 2572 DNA Homo sapiens misc_feature Incyte ID No 021667CB1 73 gtgcgtaaca cacatcaaga cagaacctgt tgccattttc agccaccaga gtgaaacgac 60 tgcccctcct ccggccccga cccaggccct ccctgagttc accagtatat tcagctcaca 120 ccagaccgca gctccagagg tgaacaatat tttcatcaaa caagaacttc ctacaccaga 180 tcttcatctt tctgtcccta cccagcaggg ccacctgtac cagctactga atacaccgga 240 tctagatatg cccagttcta caaatcagac agcagcaatg gacactctta atgtttctat 300 gtcagctgcc atggcaggcc ttaacacaca cacctctgct gttccgcaga ctgcagtgaa 360 acaattccag ggcatgcccc cttgcacata cacaatgcca agtcagtttc ttccacaaca 420 ggccacttac tttcccccgt caccaccaag ctcagagcct ggaagtccag atagacaagc 480 agagatgctc cagaatttaa ccccacctcc atcctatgct gctacaattg cttctaaact 540 ggcaattcac aatccaaatt tacccaccac cctgccagtt aactcacaaa acatccaacc 600 tgtcagatac aatagaagga gtaaccccga tttggagaaa cgacgcatcc actactgcga 660 ttaccctggt tgcacaaaag tttataccaa gtcttctcat ttaaaagctc acctgaggac 720 tcacactggt gaaaagccat acaagtgtac ctgggaaggc tgcgactgga ggttcgcgcg 780 atcggatgag ctgacccgcc actaccggaa gcacacaggc gccaagccct tccagtgcgg 840 ggtgtgcaac cgcagcttct cgcgctctga ccacctggcc ctgcatatga agaggcacca 900 gaactgagca ctgcccgtgt gacccgttcc aggtcccctg ggctccctca aatgacagac 960 ctaactattc ctgtgtaaaa acaacaaaaa caaacaaaag caagaaaacc acaactaaaa 1020 ctggaaatgt atattttgta tatttgagaa aacagggaat acattgtatt aataccaaag 1080 tgtttggtca ttttaagaat ctggaatgct tgctgtaatg tatatggctt tactcaagca 1140 gatctcatct catgacaggc agccacgtct caacatgggt aaggggtggg ggtggagggg 1200 agtgtgtgca gcgtttttac ctaggcacca tcatttaatg tgacagtgtt cagtaaacaa 1260 atcagttggc aggcaccaga agaagaatgg attgtatgtc aagattttac ttggcattga 1320 gtagtttttt tcaatagtag gtaattcctt agagatacag tatacctggc aattcacaaa 1380 tagccattga acaaatgtgt gggtttttaa aaattatata catatatgag ttgcctatat 1440 ttgctattca aaattttgta aatatgcaaa tcagctttat aggtttatta caagtttttt 1500 aggattcttt tggggaagag tcataattct tttgaaaata accatgaata cacttacagt 1560 taggatttgt ggtaaggtac ctctcaacat taccaaaatc atttctttag agggaaggaa 1620 taatcattca aatgaacttt aaaaaagcaa atttcatgca ctgattaaaa taggattatt 1680 ttaaatacaa aaggcatttt atatgaatta taaactgaag agcttaaaga tagttacaaa 1740 atacaaaagt tcaacctctt acaataagct aaacgcaatg tcatttttaa aaagaaggac 1800 ttagggtgtc gttttcacat atgacaatgt tgcatttatg atgcagtttc aagtaccaaa 1860 acgttgaatt gatgatgcag ttttcatata tcgagatgtt cgctcgtgca gtactgttgg 1920 ttaaatgaca atttatgtgg attttgcatg taatacacag tgagacacag taattttatc 1980 taaattacag tgcagtttag ttaatctatt aatactgact cagtgtctgc ctttaaatat 2040 aaatgatatg ttgaaaactt aaggaagcaa atgctacata tatgcaatat aaaatagtaa 2100 tgtgatgctg atgctgttaa ccaaagggca gaataaataa gcaaaatgcc aaaaggggtc 2160 ttaattgaaa tgaaaattta attttgtttt taaaatattg tttatcttta tttattttgt 2220 ggtaatatag taagtttttt tagaagacaa ttttcataac ttgataaatt atagttttgt 2280 ttgttagaaa agttgctctt aaaagatgta aatagatgac aaacgatgta aataattttg 2340 taagaggctt caaaatgttt atacgtggaa acacacctac atgaaaagca gaaatcggtt 2400 gctgttttgc ttctttttcc ctcttatttt tgtattgtgg tcatttccta tgcaaataat 2460 ggagcaaaca gctgtatagt tgtagaattt tttgagagaa tgagatgttt atatattaac 2520 gacaattttt tttttggaaa ataaaaagtg cctaaaagac aaaaaaaaaa aa 2572 74 219 PRT Homo sapiens misc_feature Incyte ID No 021667CD1 74 Met Pro Ser Ser Thr Asn Gln Thr Ala Ala Met Asp Thr Leu Asn 1 5 10 15 Val Ser Met Ser Ala Ala Met Ala Gly Leu Asn Thr His Thr Ser 20 25 30 Ala Val Pro Gln Thr Ala Val Lys Gln Phe Gln Gly Met Pro Pro 35 40 45 Cys Thr Tyr Thr Met Pro Ser Gln Phe Leu Pro Gln Gln Ala Thr 50 55 60 Tyr Phe Pro Pro Ser Pro Pro Ser Ser Glu Pro Gly Ser Pro Asp 65 70 75 Arg Gln Ala Glu Met Leu Gln Asn Leu Thr Pro Pro Pro Ser Tyr 80 85 90 Ala Ala Thr Ile Ala Ser Lys Leu Ala Ile His Asn Pro Asn Leu 95 100 105 Pro Thr Thr Leu Pro Val Asn Ser Gln Asn Ile Gln Pro Val Arg 110 115 120 Tyr Asn Arg Arg Ser Asn Pro Asp Leu Glu Lys Arg Arg Ile His 125 130 135 Tyr Cys Asp Tyr Pro Gly Cys Thr Lys Val Tyr Thr Lys Ser Ser 140 145 150 His Leu Lys Ala His Leu Arg Thr His Thr Gly Glu Lys Pro Tyr 155 160 165 Lys Cys Thr Trp Glu Gly Cys Asp Trp Arg Phe Ala Arg Ser Asp 170 175 180 Glu Leu Thr Arg His Tyr Arg Lys His Thr Gly Ala Lys Pro Phe 185 190 195 Gln Cys Gly Val Cys Asn Arg Ser Phe Ser Arg Ser Asp His Leu 200 205 210 Ala Leu His Met Lys Arg His Gln Asn 215 75 5325 DNA Homo sapiens misc_feature Incyte ID No 224855.4 75 acctcgcact ctcagtttca ccgctcgatc ttgggaccca ccgctgccct cagctccgag 60 tccagggcga gtgcagagca gagcgggcgg aggaccccgg gcgcgggcgc ggacggcacg 120 cggggcatga acctggaggg cggcggccga ggcggagagt tcggcatgag cgcggtgagc 180 tgcggcaacg ggaagctccg ccagtggctg atcgaccaga tcgacagcgg caagtacccc 240 gggctggtgt gggagaacga ggagaagagc atcttccgca tcccctggaa gcacgcgggc 300 aagcaggact acaaccgcga ggaggacgcc gcgctcttca aggcttgggc actgtttaaa 360 ggaaagttcc gagaaggcat cgacaagccg gaccctccca cctggaagac gcgcctgcgg 420 tgcgctttga acaagagcaa tgactttgag gaactggttg agcggagcca gctggacatc 480 tcagacccgt acaaagtgta caggattgtt cctgagggag ccaaaaaagg agccaagcag 540 ctcaccctgg aggacccgca gatgtccatg agccacccct acaccatgac aacgccttac 600 ccttcgctcc cagcccaggt tcacaactac atgatgccac ccctcgaccg aagctggagg 660 gactacgtcc cggatcagcc acacccggaa atcccgtacc aatgtcccat gacgtttgga 720 ccccgcggcc accactggca aggcccagct tgtgaaaatg gttgccaggt gacaggaacc 780 ttttatgctt gtgccccacc tgagtcccag gctcccggag tccccacaga gccaagcata 840 aggtctgccg aagccttggc gttctcagac tgccggctgc acatctgcct gtactaccgg 900 gaaatcctcg tgaaggagct gaccacgtcc agccccgagg gctgccggat ctcccatgga 960 catacgtatg acgccagcaa cctggaccag gtcctgttcc cctacccaga ggacaatggc 1020 cagaggaaaa acattgagaa gctgctgagc cacctggaga ggggcgtggt cctctggatg 1080 gcccccgacg ggctctatgc gaaaagactg tgccagagca ggatctactg ggacgggccc 1140 ctggcgctgt gcaacgaccg gcccaacaaa ctggagagag accagacctg caagctcttt 1200 gacacacagc agttcttgtc agagctgcaa gcgtttgctc accacggccg ctccctgcca 1260 agattccagg tgactctatg ctttggagag gagtttccag accctcagag gcaaagaaag 1320 ctcatcacag ctcacgtaga acctctgcta gccagacaac tatattattt tgctcaacaa 1380 aacagtggac atttcctgag gggctacgat ttaccagaac acatcagcaa tccagaagat 1440 taccacagat ctatccgcca ttcctctatt caagaatgaa aaatgtcaag atgagtgggn 1500 nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn 1560 nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn 1620 nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn 1680 nnnnnnnnnn nnnnnnnnnc attgtaaata tttgacttta gtgaaagcgt ccaattgact 1740 gcgcctctta ctgttttgag gaactcagaa gtggagattt cagttcagcg gttgaggaga 1800 attgcggcga gacaagcatg gaaaatcagt gacatctgat tggcagatga gcttatttca 1860 aaaggaaggg tggctttgca ttttcttgtg ttctgtagac tgccatcatt gatgatcact 1920 gtgaaaattg accaagtgat gtgtttacat ttactgaaat gcgctcttta atttgttgta 1980 gattaggtct tgctggaaga cagagaaaac ttgcctttca gtattgacac tgactagagt 2040 gatgactgct tgtaggtatg tctgtgccat ttctcaggga agtaagatgt aaattgaaga 2100 agcctcacac gtaaaagaaa tgtattaatg tatgtaggag ctgcagttct tgtggaagac 2160 acttgctgag tgaaggaaat gaatctttga ctgaagccgt gcctgtagcc ttggggaggc 2220 ccatccccca cctgccagcg gtttcctggt gtgggtccct ctgccccacc ctccttccca 2280 ttggctttct ctccttggcc tttcctggaa gccagttagt aaacttccta ttttcttgag 2340 tcaaaaaaca tgagcgctac tcttggatgg gacatttttg tctgtcctac aatctagtaa 2400 tgtctaagta atggttaagt tttcttgttt ctgcatcttt ttgaccctca ttctttagag 2460 atgctaaaat tcttcgcata aagaagaaga aattaaggaa cataaatctt aatacttgaa 2520 ctgttgccct tctgtccaag tacttaacta tctgttccct tcctctgtgc cacgctcctc 2580 tgtttgtttg gctgtccagc gatcagccat ggcgacacta aaggaggagg agccggggac 2640 tcccaggctg gagagcactg ccaggaccca ccactggaag caggatggag ctgactacgg 2700 aactgcacac tcagtgggct gtttctgctt atttcatctg ttctatgctt cctcgtgcca 2760 attatagttt gacagggcct taaaattact tggctttttc caaatgcttc tatttataga 2820 atcccaaaga cctccacttg cttaagtata cctatcactt acatttttgt ggttttgaga 2880 aagtacagca gtagactggg gcgtcacctc caggccgttt ctcatactac aggatattta 2940 ctattactcc caggatcagc agaagattgc gtagctctca aatgtgtgtt cctgcttttc 3000 taatggatat tttaaattca ttcaacaagc acctagtaag tgcctgctgt atccctacat 3060 tacacagttc agcctttatc aagcttagtg agcagtgagc actgaaacat tattttttaa 3120 tgtttaaaaa gtttctaata ttaaagtcag aatattaata caattaatat taatattaac 3180 tacagaaaag acaaacagta gagaacagca aaaaaataaa aaggatctcc ttttttccca 3240 gcccaaattc tcctctctaa aagtgtccac aagaaggggt gtttattctt ccaacacatt 3300 tcacttttct gtaaatatac ataaacttaa aaagaaaacc tcatggagtc atcttgcaca 3360 cactttcatg cagtgctctt tgtagctaac agtgaagatt tacctcgttc tgctcagagg 3420 ccttgctgtg gagctccact gccatgtacc cagtagggtt tgacatttca ttagccatgc 3480 aacatggata tgtattgggc agcagactgt gtttcgtgaa ctgcagtgat gtatacatct 3540 tatagatgca aagtattttg gggtatatta tcctaaggga agataaagat gatattaaga 3600 actgctgttt cacggggccc ttacctgtga ccctctttgc tgaagaatat ttaaccccac 3660 acagcacttt caaagaagct gtcttggaag tctgtctcag gagcaccctg tcttcttaat 3720 tctccaagcg gatgctccat ttcaattgct ttgtgacttc ttcttctttg tttttttaaa 3780 tattatgctg ctttaacagt ggagctgaat tttctggaaa atgcttcttg gctggggcca 3840 ctacctcctt tcctatcttt acatctatgt gtatgttgac tttttaaaat tctgagtgat 3900 ccagggtatg acctagggaa tgaactagct atgaaatact cagggttagg aatcctagca 3960 cttgtctcag gactctgaaa aggaacggct tcctcattcc ttgtcttgat aaagtggaat 4020 tggcaaacta gaatttagtt tgtactcagt ggacagtgct gttgaagatt tgaggacttg 4080 ttaaagagca ctgggtcata tggaaaaaat gtatgtgtct cccaggtgca tttcttggtt 4140 tatgtcttgt tcttgagatt ttgtatattt aggaaaacct caagcagtaa ttaatatctc 4200 ctggaacact atagagaacc aagtgaccga ctcatttaca actgaaacct aggaagcccc 4260 tgagtcctga gcgaaaacag gagagttagt cgccctacag gaaacccagc tagactattg 4320 ggtatgaact aaaaagagac tgtgccatgg tgagaaaaat gtaaaatcct acagtggaat 4380 gagcagccct tacagtgttg ttaccaccaa gggcaggtag gtattagtgt ttgaaaaagc 4440 tggtctttga gcgagggcat aaatacagct agccccaggg gtggaacaac tctgggagtc 4500 ttgggtactc gcacctcttg gctttgttga tgctccgcca ggaaggccac ttgtgtgtgc 4560 gtgtcagtta cttttttagt aacaattcag atccagtgta aacttccgtt cattgctctc 4620 cagtcacatg cccccacttc cccacaggtg aaagtttttc tgaaagtgtt gggattggtt 4680 aaggtcttta tttgtattac gtatctcccc aagtcctctg tggccagctg cgtctgtctg 4740 aatggtgcgt gaaggctctc agaccttaca caccattttg taagttatgt tttacatgcc 4800 ccgtttttga gactgatctc gatgcaggtg gatctccttg agatcctgat agcctgttac 4860 aggaatgaag taaaggtcag ttttttttgt attgattttc acagctttga ggaacatgca 4920 taagaaatgt agctgaagta gagggggcgt gagagaaggg ccaggccggc aggccaaccc 4980 tcctccaatg gaaattcccg tgttgcttca aactgagaca gatgggactt aacaggcaat 5040 ggggtccact tccccctctt cagcatcccc cgtaccccac tttctgctga aagaactgcc 5100 agcaggtagg accccagagg cccccaaatg aaagcttgaa tttcccctac tggctctgcg 5160 ttttgctgag atctgtagga aaggatgctt cacaaactga ggtagataat gctatgctgt 5220 cgttggtata catcatgaat ttttatgtaa attgctctgc aaagcaaatt gatatgtttg 5280 ataaatttat gtttttaggt aaataaaaac ttttaaaaag ttgtt 5325 76 2278 DNA Homo sapiens misc_feature Incyte ID No 1518310CB1 76 ggctcctctc cccgactcgg agcccctcgg cggcgcccgg cccaggaccc gcctaggagc 60 gcaggagccc cagcgcagag accccaacgc cgagaccccc gccccggccc cgccgcgctt 120 cctcccgacg cagagcaaac cgcccagagt agaagatgga ttggggcacg ctgcagacga 180 tcctgggggg tgtgaacaaa cactccacca gcattggaaa gatctggctc accgtcctct 240 tcatttttcg cattatgatc ctcgttgtgg ctgcaaagga ggtgtgggga gatgagcagg 300 ccgactttgt ctgcaacacc ctgcagccag gctgcaagaa cgtgtgctac gatcactact 360 tccccatctc ccacatccgg ctatgggccc tgcagctgat cttcgtgtcc acgccagcgc 420 tcctagtggc catgcacgtg gcctaccgga gacatgagaa gaagaggaag ttcatcaagg 480 gggagataaa gagtgaattt aaggacatcg aggagatcaa aacccagaag gtccgcatcg 540 aaggctccct gtggtggacc tacacaagca gcatcttctt ccgggtcatc ttcgaagccg 600 ccttcatgta cgtcttctat gtcatgtacg acggcttctc catgcagcgg ctggtgaagt 660 gcaacgcctg gccttgtccc aacactgtgg actgctttgt gtcccggccc acggagaaga 720 ctgtcttcac agtgttcatg attgcagtgt ctggaatttg catcctgctg aatgtcactg 780 aattgtgtta tttgctaatt agatattgtt ctgggaagtc aaaaaagcca gtttaacgca 840 ttgcccagtt gttagattaa gaaatagaca gcatgagagg gatgaggcaa cccgtgctca 900 gctgtcaagg ctcagtcgct agcatttccc aacacaaaga ttctgacctt aaatgcaacc 960 atttgaaacc cctgtaggcc tcaggtgaaa ctccagatgc cacaatggag ctctgctccc 1020 ctaaagcctc aaaacaaagg cctaattcta tgcctgtctt aattttcttt cacttaagtt 1080 agttccactg agaccccagg ctgttagggg ttattggtgt aaggtacttt catattttaa 1140 acagaggata tcggcatttg tttctttctc tgaggacaag agaaaaaagc caggttccac 1200 agaggacaca gagaaggttt gggtgtcctc ctggggttct ttttgccaac tttccccacg 1260 ttaaaggtga acattggttc tttcatttgc tttggaagtt ttaatctcta acagtggaca 1320 aagttaccag tgccttaaac tctgttacac tttttggaag tgaaaacttt gtagtatgat 1380 aggttatttt gatgtaaaga tgttctggat accattatat gttccccctg tttcagaggc 1440 tcagattgta atatgtaaat ggtatgtcat tcgctactat gatttaattt gaaatatggt 1500 cttttggtta tgaatacttt gcagcacagc tgagaggctg tctgttgtat tcattgtggt 1560 catagcacct aacaacattg tagcctcaat cgagtgagac agactagaag ttcctagtga 1620 tggcttatga tagcaaatgg cctcatgtca aatatttaga tgtaattttg tgtaagaaat 1680 acagactgga tgtaccacca actactacct gtaatgacag gcctgtccaa cacatctccc 1740 ttttccatga ctgtggtagc cagcatcgga aagaacgctg atttaaagag gtcgcttggg 1800 aattttattg acacagtacc atttaatggg gaggacaaaa tggggcaggg gagggagaag 1860 tttctgtcgt taaaaacaga tttggaaaga ctggactcta aattctgttg attaaagatg 1920 agctttgtct acttcaaaag tttgtttgct taccccttca gcctccaatt ttttaagtga 1980 aaatataact aataacatgt gaaaagaata gaagctaagg tttagataaa tattgagcag 2040 atctatagga agattgaacc tgaatattgc cattatgctt gacatggttt ccaaaaaatg 2100 gtactccaca tacttcagtg agggtaagta ttttcctgtt gtcaagaata gcattgtaaa 2160 agcattttgt aataataaag aatagcttta atgatatgct tgtaactaaa ataattttgt 2220 aatgtatcaa atacatttaa aacattaaaa tataatctct atagtaacga acagaaaa 2278 77 226 PRT Homo sapiens misc_feature Incyte ID No 1518310CD1 77 Met Asp Trp Gly Thr Leu Gln Thr Ile Leu Gly Gly Val Asn Lys 1 5 10 15 His Ser Thr Ser Ile Gly Lys Ile Trp Leu Thr Val Leu Phe Ile 20 25 30 Phe Arg Ile Met Ile Leu Val Val Ala Ala Lys Glu Val Trp Gly 35 40 45 Asp Glu Gln Ala Asp Phe Val Cys Asn Thr Leu Gln Pro Gly Cys 50 55 60 Lys Asn Val Cys Tyr Asp His Tyr Phe Pro Ile Ser His Ile Arg 65 70 75 Leu Trp Ala Leu Gln Leu Ile Phe Val Ser Thr Pro Ala Leu Leu 80 85 90 Val Ala Met His Val Ala Tyr Arg Arg His Glu Lys Lys Arg Lys 95 100 105 Phe Ile Lys Gly Glu Ile Lys Ser Glu Phe Lys Asp Ile Glu Glu 110 115 120 Ile Lys Thr Gln Lys Val Arg Ile Glu Gly Ser Leu Trp Trp Thr 125 130 135 Tyr Thr Ser Ser Ile Phe Phe Arg Val Ile Phe Glu Ala Ala Phe 140 145 150 Met Tyr Val Phe Tyr Val Met Tyr Asp Gly Phe Ser Met Gln Arg 155 160 165 Leu Val Lys Cys Asn Ala Trp Pro Cys Pro Asn Thr Val Asp Cys 170 175 180 Phe Val Ser Arg Pro Thr Glu Lys Thr Val Phe Thr Val Phe Met 185 190 195 Ile Ala Val Ser Gly Ile Cys Ile Leu Leu Asn Val Thr Glu Leu 200 205 210 Cys Tyr Leu Leu Ile Arg Tyr Cys Ser Gly Lys Ser Lys Lys Pro 215 220 225 Val 78 445 DNA Homo sapiens misc_feature Incyte ID No 098533.1 78 ggcaaggcca gtggctccgc cgctgggtcc gctgcccttt actttcagtc agcctggggc 60 ggtgtcctct cctacagaag tcctgagcgg ccttccacgt ggccggccct cgagtccgtc 120 cgccccgacc cttcgtagtc ccgaaaccgc ccccctggct aaggtctctt tcccccaggc 180 tgcttccttt ctccttgctt ttttcccacc ttttttgtta ctgaccaagg tgaatccttt 240 ccttaacaaa tcggcttaaa gcaagctaac tcagttacaa tacagtagaa ctgtacttaa 300 aaaaaaaaga aacgtgaatc taaccgttac gtcagaaaaa aaaatcttaa attagacgaa 360 tttcaaacag tgcttaacac atcgcagagc atttgcagtt atttgnatca cgncttttga 420 aacaccttta tgctgtaaat agagc 445 79 5227 DNA Homo sapiens misc_feature Incyte ID No 410785.1 79 cacaagacct ggaattgaca ggactcccaa ctagtacaat gacagaagat aaggtcactg 60 ggaccctggt tttcactgtc atcactgctg tgctgggttc cttccagttt ggatatgaca 120 ttggtgtgat caatgcacct caacaggtaa taatatctca ctatagacat gttttgggtg 180 ttccactgga tgaccgaaaa gctatcaaca actatgttat caacagtaca gatgaactgc 240 ccacaatctc atactcaatg aacccaaaac caaccccttg ggctgaggaa gagactgtgg 300 cagctgctca actaatcacc atgctctggt ccctgtctgt atccagcttt gcagttggtg 360 gaatgactgc atcattcttt ggtgggtggc ttggggacac acttggaaga atcaaagcca 420 tgttagtagc aaacattctg tcattagttg gagctctctt gatggggttt tcaaaattgg 480 gaccatctca tatacttata attgctggaa gaagcatatc aggactatat tgtgggctaa 540 tttcaggcct ggttcctatg tatatcggtg aaattgctcc aaccgctctc aggggagcac 600 ttggcacttt tcatcagctg gccatcgtca cgggcattct tattagtcag attattggtc 660 ttgaatttat cttgggcaat tatgatctgt ggcacatctt gcttggcctg tctggtgtgc 720 gagccatcct tcagtctctg ctactctttt tctgtccaga aagccccaga tacctttaca 780 tcaagttaga tgaggaagtc aaagcaaaac aaagcttgaa aagactcaga ggatatgatg 840 atgtcaccaa agatattaat gaaatgagaa aagaaagaga agaagcatcg agtgagcaga 900 aagtctctat aattcagctc ttcaccaatt ccagctaccg acagcctatt ctagtggcac 960 tgatgctgca tgtggctcag caattttccg gaatcaatgg cattttttac tactcaacca 1020 gcatttttca gacggctggt atcagcaaac ctgtttatgc aaccattgga gttggcgctg 1080 taaacatggt tttcactgct gtctctgtat tccttgtgga gaaggcaggg cgacgttctc 1140 tctttctaat tggaatgagt gggatgtttg tttgtgccat cttcatgtca gtgggacttg 1200 tgctgctgaa taagttctct tggactgagt tactgtgagc atgatagcca tcttcctctt 1260 tgtcagcttc tttgaaattg ggccaggccc gatcccctgg ttcatggtgg ctgagttttt 1320 cagtcaagga ccacgtcctg ctgctttagc aatagctgca ttcagcaatt ggacctgcaa 1380 tttcattgta gctctgtgtt tccagtacat tgcggacttc tgtggacctt atgtgttttt 1440 cctctttgct ggagtgctcc tggcctttac cctgtttaca ttttttaaag ttccagaaac 1500 caaaggaaag tcttttgagg aaattgctgc agaattccaa aagaagagtg gctcagccca 1560 caggccaaaa gctgctgtag aaatgaaatt cctaggagct acagagactg tgtaaaaaaa 1620 aaaccctgct ttttgacatg aacagaaaca ataagggaac cgtctgtttt taaatgatga 1680 ttccttgagc attttatatc cacatcttta agtattgttt tatttttatg tgctctcatc 1740 agaaatgtca tcaaatatta ccaaaaaagt atttttttaa gttagagaat atatttttga 1800 tggtaagact gtaattaagt aaaccaaaaa ggctagttta ttttgttaaa ctaaagggca 1860 ggtggttcta atatttttag ctctgttctt tataacaagg ttcttctaaa attgaagaga 1920 tttcaacata tcattttttt aacacataac tagaaacctg aggatgcaac aaatatttat 1980 atatttgaat atcattaaat tggaattttc ttacccatat atcttatgtt aaaggagata 2040 tggctagtgg caataagttc catgttaaaa tagacaactc ttccatttat tgcactcagc 2100 ttttttcttg agtactagaa tttgtatttt gcttaaaatt ttacttttgt tctgtatttt 2160 catgtggaat ggattataga gtatactaaa aaatgtctat agagaaaaac tttcattttt 2220 ggtaggctta tcaaaatctt tcagcactca gaaaagaaaa ccattttagt tcctttattt 2280 aatggccaaa tggtttttgc aagatttaac actaaaaagg tttcacctga tcatatagcg 2340 tgggttatca gttaacatta acatctatta taaaaccatg ttgattccct tctggtacaa 2400 tcctttgagt tatagtttgc tttgcttttt aattgaggac agcctggttt tcacatacac 2460 tcaaacatca tgagtcagac atttggtata ttacctcaat tcctaataag tttgatcaat 2520 ctaatgtaag aaaatttgaa gtaaaggatt gatcactttg ttaaaaatat tttctgaatt 2580 attatgtctc aaaataagtt gaaaaggtag ggtttgagga ttcctgagtg tgggcttctg 2640 aaacttcata aatgttcagc ttcagacttt tatcaaaatc cctatttaat tttcctggaa 2700 agactgattg ttttatggtg tgttcctaac ataaaataat cgtctccttt gacatttcct 2760 tctttgtctt agctgtatac agattctagc caaactattc tatggccatt actaacacgc 2820 attgtacact atctatctgc ctttacctac ataggcaaat tggaaataca cagatgatta 2880 aacagacttt agcttacagt caattttaca attatggaaa tatagttctg atgggtccca 2940 aaagcttagc agggtgctaa cgtatctcta ggctgttttc tccaccaact ggagcactga 3000 tcaatccttc ttatgtttgc tttaatgtgt attgaagaaa agcacttttt aaaaagtact 3060 ctttaagagt gaaataatta aaaaccactg aacatttgct ttgttttcta aagttgttca 3120 catatatgta atttagcagt ccaaagaaca agaaattgtt tcttttcagt gtgatttgtt 3180 tttcatttgg gccaatttgg gataaactat tttcacttgg gatttcagga tacagtcaaa 3240 ataagcttaa ataactcagg acatctttgt gctaaactgt gaactctgga caaaaataga 3300 gagtctctga atagggcagg agcaggaaaa tggctcctgg gtggctcttg tatgcttctt 3360 caggatgctg atggcctttg ggaagcccag tgtaaacaat gataaaggag cttaacactt 3420 ttataggtga tacatgtgat ttaatcaaat cactattcct gatctcattt actaacagaa 3480 taaagtggta aatatttaaa ttaaaaattc caaagaccac ttttaagtgc ttcttcacta 3540 ttttgactgg cccacaaaca ccagaaattc agaccctgaa gttttctgcc tcagagaaat 3600 ttaagtacct tatattgttc cccttctaca actttttcct tgcagagata catgtgagtt 3660 gacaagaaac attaaaggga aataagaaga agctgataaa gctttatagg aggaccaaag 3720 aactagctta ctataataaa aaaattttaa gtcttcaagg gtatacatca taataaaaaa 3780 taaaattgac agtaattaat taaatttaat cccagggaaa ttagatgtga atttgaacac 3840 ctaactttcc atgtactctc tcatttttgt ggaagtgttt ctatactcta atgcctttac 3900 aaatgtgatt tttctcttag ctcgtttgaa gtatgagaat tagagttttt ggtctcgcat 3960 tcacctgcta catctaggat tgcccactgt catgactccc agggaaaagg tcctatctta 4020 gcttcctcct ccctactttc ctctacatgg tcagcactgt aatgtagcta agatatagta 4080 aggcattgct ccctccccct acacttcaag gagttcacag tctaatgggg agttcaggaa 4140 ggccagagta ttaatatccc catctgtgtc ttttgccttc catgaacctg ggttttgagc 4200 cctctcttgt aaaatgggca cagtaatatt acctacctca gggagttgtg aggattaaac 4260 atgaagtgct aagcatagtg cctggtacaa agacagtact caataagtgc tacctaaaac 4320 tagtattcat agcaatactg ttaggataaa gaattatcat atatgagata gttccaaatt 4380 tttgtttttt taaaaaaaaa agagttttat aagttcaaga taatattttc ttacttcaaa 4440 gaaacaatct cacaacgagg gaatggtaag aatcaggaga gattactaac ctggcagagg 4500 agctatcaca atcacaaagg tggtttttcc agggcacggc tcatccatta cactccagat 4560 gtgctgaccc ctgccatttc cccaaatgtg ggaaacccaa ctgcacagtt tgtagtagtg 4620 ggtgactgtg ttcatgcgct cccctgaaaa caacaacaac aacaaagaat cagaagagat 4680 actaggctat ctaattccta aatccaaacc tgatatttct aagtaagatt ataagaattt 4740 ttattgcatt ttctgaattt gcttttgcat aagttatgtt atttttacag ggtctatatt 4800 actattattt cttagaataa tactaattat aaaacaaaat tctgtatatc acatttaaat 4860 gtaatttaat agaattataa tcacaagaca agaccaaact ttgtgtgata atcctcagta 4920 attgcganag gggnatatnc atgnaggcca gcatacatgc ataaactact tcntattgct 4980 aggctaattg tnccatatgt agcaaataca gcagttcagc aatatcttgt gcttacaggg 5040 tcctaagcag aggtgatgag tcaagtgtaa atatatatat atattttttt atttttcatg 5100 gcaattgtat attagtaacc tggggagaaa aggtttattg acaaccactc tgatccatct 5160 gctgctattt ttactgctaa tttggtgcac attaaaaaga atgatcatga aaagatatta 5220 ctttgag 5227 80 1199 DNA Homo sapiens misc_feature Incyte ID No 1089210.1 80 aaggaaacag gatctgctta gtgaaagaag tggcaagcaa tggatcccaa atatcagcgt 60 gtagagctaa atgatggtca cttcatgccc gtattgggat ttggcaccta tgcacctcca 120 gaggttccga ggaacagagc tgtggaggtc accaaattag caatagaagc tggcttccgc 180 catattgatt ctgcttattt atacaataat gaggagcagg ttggactggc catccgaagc 240 aagattgcag atggcagtgt gaagagagaa gacatattct acacttcaaa gctttggtgc 300 actttctttc aaccacagat ggtccaacca gccttggaaa gctcactgaa aaaactttaa 360 ctggactatg ttgacctcta tcttcttcat ttcccaatgg ctctcaagcc aggtgagacg 420 ccactaccaa aagatgaaaa tggaaaagta atattcgaca cagtggatct ctctgccaca 480 tgggaggtca tggagaagtg taaggatgca ggattggcca agtccatcgg ggtgtcaaac 540 ttcaactgca ggcagctgga gatgatcctc aacaagccag gactcaagta caagcctgtc 600 tgcaaccagg tagaatgtca tccttacctc aaccagagca aactgctgga tttctgcaag 660 tcaaaagaca ttgttctggt tgcccacagt gctctgggaa cccaacgaca taaactatgg 720 gtggacccaa actccccagt tcttttggag gacccagttc tttgtgcctt agcaaagaaa 780 cacaaacgaa ccccagccct gattgccctg cgctaccagc tgcagcgtgg ggttgtggtc 840 ctggccaaga gctacaatga gcagcggatc agagagaaca tccaggtttt tgaattccag 900 ttgacatcag agggatatga aagttctaga tggtctaaac agaaattatc gatatgttgt 960 catggatttt cttatggacc atcctgatta tccattttca gatgaatatt agcatagagg 1020 gtgttgcacg acatctagca gaaggccctg tgtgtggatg gtgatgcaga ggatgtctct 1080 atgctggtga ctggacacac ggcctctggt taaatccctc ccctcctgct tggcaacttc 1140 agctagctag atatatccat ggtccagaaa gcaaacataa taaattttta tcttgaagt 1199 81 807 DNA Homo sapiens misc_feature Incyte ID No 333453.6 81 gaacaagact ccgtcaaaaa aaaaaaaatt gnttnggaac ctggttctgg aatcggcttg 60 aatcattcca gcctttcata cttatagctg tgtggccttg ggcaacttac ttaactttat 120 ctataaaatg gggacaatag cttctcttcc tcatagcatg gttgtnagga ttagatgaag 180 ttctcagtgg gcattcctgt aagctctagg gagatgttag ctgttactaa tgtttggcac 240 catgacaaat gattagatgg aactttggag caattaataa tacaaattaa aataagggga 300 caaagccagc caaggagaaa agtaaaagat ccaagaatag gggcatataa tggctttatt 360 tttccttgag tctagtgtga ttctaacacc tgagtccaac cattcattat gtaggtccgt 420 atcctctcct gttcttttcc tctcatcctg ggtaccagac agaaggaaaa actgaaacaa 480 atgatgagtc ggctcccttt ctttccttcc atggtggcta tttaggtggc tgatttatga 540 agaacctgga tttcagggtg ttcctttcat cctggaacct ggtgaatacc ctgacttgtc 600 cttctgggat acagaagcag cgtacattgg atccatgcgg cctctgaaaa tggtaaaaat 660 gaaatccaaa tgtccttgtg gtgattcttt gtcagcttga cgtggtaatt cacagggtgt 720 gactttgaag caataaagct gacttttaag acacaaattt gtagtagatt ggacctattg 780 ctcaatacaa atcatggaaa gcataac 807 82 764 DNA Homo sapiens misc_feature Incyte ID No 365070.1 82 acgaagcagc tgactgtgca tcacgcagtc acaatattgt ttttagggtg agggtggagg 60 actgtgtgtc cgtggattac tcctcctgct ggtggattgc agatgcatta ttaggtcata 120 ctggctagaa tgcagctttt ctcccaccat aacatgaaaa cagtgtaaga acatagggtg 180 ctttgtgcat agcccttctc tatgtaagca gccatggcag tcattaaaga gaaaggagta 240 gctttgacat taagctcccc agatccctgc tgctcatact tctggcaagg ggttcccctc 300 tctcatgcat gaacaggggc atccaaaata agaagctctc cattctgtgg tggggaaagc 360 ggagagggga gtgggtgaag ctgggaaagt aaaggcagca cgttacagaa ggaagaaagg 420 aagccagtaa ctgagggccc actgcctgcc cggccctggg ccaggccctc aacagaagcc 480 atctcattta agccctgcaa ccaatgagat gcacgtcatc attggctctt acagacaaga 540 aaactagact cagaggggct gagtccacat cccagacagc tcactgcaga cacaggtgga 600 gtggttccta caagacatcc agttttaaca acaaaagagt tattgaaatg catgggtaga 660 aattgaacca ggaaaatcag taaagtgatt gtaaaaaaga aggactagct tgcctggaga 720 tgatgtttct tgcttttgga aaaaaaaaaa aggtctctga aatt 764 83 1325 DNA Homo sapiens misc_feature Incyte ID No 365070.3 83 gcgctgctgg cggccccggc ggccgggcgt gctgcctgca agatgtccgt gcgccgcggc 60 cggcggccgg cgcggccggg gacccgcctc tcctggctgc tgtgctgcag cgccctgctg 120 tccccggccg cgggctacgt gatcgtgagc tccgtgtctt gggccgtcac caacgaggtg 180 gacgaggagc tggacagcgc ctccactgag gaggctatgc ccgcgctgct agaggattcg 240 ggcagcatct ggcagcaaag cttccccgcc tctgcccaca aggaggacgc gcacctgcgg 300 ccccgggcgg gcgccgcccg ggccaggccg ccccccgcgc cacccgggat gttctcctac 360 cggcgcgagg gcggccagac ggccagtgcg cccccgggcc ctagactgcg cgccgccacc 420 gcccgctccc tggcccatgc cagcgtctgg ggctgcctgg ccaccgtgtc cacccacaag 480 aagatccaag gactgccatt tgggaactgc ctgcccgtca gtgatggccc cttcaacaat 540 agcactggga ttcctttctt ctacatgaca gccaaggacc ccgtggtggc tgatctgatg 600 aagaacccca tggcctcgct gatgctgcca gaatcagaag gggagttctg cagaaaaaac 660 atcgttgatc cggaagatcc ccgatgtgtc cagttaacgc tcactggcca gatgatcgca 720 gtgtctccag aagaagtaga atttgccaag caagccatgt tttcaaggca cccagggatg 780 aggaagtggc ctcgtcaata tgaatggttc tttatgaaga tgaggataga acatatctgg 840 cttcagaaat ggtatggagg cgcatccagt atttcaaggg aggaatattt caaagcagtt 900 cccagaaagg cctgatggag tgagaagaaa gtccttggtg tttgcactta aataaaaacc 960 ttttcagtga tgcagccaga cagctattga ccactgtctc tttgttgaag ggttcatagc 1020 agccctgcca tccctgcagc agaatgagag agggtgaaca gggaactcta tgctagattt 1080 gagattaaag tggtcatttg cagatctcca actcacacag atacttcacg tagatagtct 1140 ttattccatt gtattcaatc cagactcatc gattcagaaa tcatataata gctggtggtc 1200 aaaatgacat gttgagatca ttgttgtttc attgtttaag gnaaaaaaaa aatgcctgta 1260 cctacaatgt gattgctttg tattgtgaga gtatcttgtt gcttgctctg ccaaatgcag 1320 tcttg 1325 84 3663 DNA Homo sapiens misc_feature Incyte ID No 413921.2 84 gtgcgctagg ctccggactc cgcggcgcag actggcacct cgcagtctcc ccaggtccgc 60 ccagcagccg cgcttcagcc agaatactgg gatcttcagt ggcaggagga gtaatcagaa 120 gacggagatg aattttaaca ctattttgga ggagattctt attaaaaggt cacagcagaa 180 aaagaagaca tcgcccttaa actacaaaga gagacttttt gtacttacaa agtccatgct 240 aacctactat gagggtcgag cagagaagaa atacagaaag gggtttattg atgtttcaaa 300 aatcaagtgt gtggaaatag tgaagaatga tgatggtgtc attccctgtc aaaataagta 360 tccatttcag gttgttcatg atgctaacac actttacatt tttgcaccta gtccacaaag 420 cagggacctg tgggtgaaga agttaaaaga agaaataaag aacaacaata atattatgat 480 taaatatcat cctaaattct ggacagatgg aagttatcag tgttgtagac aaactgaaaa 540 attagcaccc ggatgtgaaa aatacaatct ttttgagagc agtataagaa aagcactacc 600 tccagcacca gaaacaaaga agcgaaggcc tcccccacca attccactag aagaagaaga 660 taatagtgaa gaaatcgttg tagccatgta tgatttccaa gcagcagaag gacatgatct 720 cagattagag agaggccaag agtatctcat tttagaaaag aatgatgtgc attggtggag 780 agcaagagat aaatatggga atgaaggata tatcccaagt aattacgtaa cgggaaagaa 840 atcaaacaac ttagatcaat atgaatggta ttgcagaaat atgaatagaa gcaaggcaga 900 gcaactcctc cgcagtgaag ataaagaagg tggttttatg gtaagggatt ccagtcaacc 960 aggcttgtac acagtctccc tttataccaa gtttggagga gaaggttcat cgggttttag 1020 gcattatcat ataaaggaaa caacaacatc tccaaagaag tattacctag ctgaaaaaca 1080 tgcttttggc tccattcctg agattattga atatcataag cacaatgcag caggacttgt 1140 caccaggctt cggtacccag ttagtgtgaa agggaagaat gcacccacca ctgcaggatt 1200 cagctatgag aaatgggaga ttaacccttc agaactgacc tttatgaggg aattgggaag 1260 tggactgttt ggagtggtga ggcttggcaa atggcgagcc cagtacaaag tcgcaatcaa 1320 agctattcgg gaaggtgcaa tgtgcgagga ggactttata gaagaagcta aagtgatgat 1380 gaagctgaca cacccgaagt tagtgcagct ttatggtgtg tgcacccagc agaaaccaat 1440 atacattgtt actgagttca tggaaagggg ctgccttctg aatttcctcc gacagagaca 1500 aggtcatttc agtagagacg tactgctgag catgtgtcag gatgtgtgtg aagggatgga 1560 gtatctggag agaaacagct tcatccacag agatctggct gccagaaatt gtctagtaag 1620 tgaggcggga gttgtaaaag tatctgattt tggaatggcc aggtatgttc tggatgatca 1680 gtacacaagt tcttctggtg ctaagtttcc tgtgaagtgg tgtccacctg aagtgtttaa 1740 ttacagccgc ttcagcagca aatcagatgt ctggtcattt ggtgttttaa tgtgggaagt 1800 attcacggaa ggcagaatgc cttttgaaaa atacaccaat tatgaagtgg taaccatggt 1860 tactcgaggc caccgactct accagccgaa gttggcgtcc aactatgtgt atgaggtgat 1920 gctgagatgt tggcaggaga aaccagaggg aaggccttct ttcgaagatc tgctgcgcac 1980 aatagatgaa ctagttgaat gtgaagaaac ttttggaaga taagtgatgt gtgaccagtg 2040 gctcccagat tcccaagcac aaggaaggat gggcattttg tggcttttaa tttattgagc 2100 acttggacat gtagatcatt ttacttatac agtggaaaca cataaataat ttgcttctag 2160 accagcctct gtctagactt gcttctagac agaatctccc agagtgtgga aatgttgcct 2220 tagaaatggt gattaaaatc actcatttct attcattcct caggcacttg agtgacagtt 2280 gtttaccagg cactgtgtgt agccccaggg tttggccatt caggggtgca cacatgggac 2340 catgttagct gatgccagtt gaaggccagg gtatttggga aggggaaggg tattagagtc 2400 atgaccaagc aacccttctt tttccctttg acttctacag aaatctgggc ctgagacatt 2460 gtctacaatt gggttctaga tacatcagga acccatcttg gataaataaa tacctatctt 2520 ttgttttgaa aacatctcag ttttcaagac tgctcttagt attacatgaa caatatttgt 2580 atgctgtata tattgtaaat atatataata tataaagtta tatatttatg agaaacacga 2640 attgtctttt aattgaaact tttaatcctg tagtatagga gttcaccttc ttaggactag 2700 agactgtgcc ttatagctgt taattcattt ccccctgaac atcaaatatg cctgaagaga 2760 agaaagtcta gattcttcta tgagtaacgc cccctcctca ctcaggtaaa tgtgtctggg 2820 gatgcctgtc cagcttaacc acgtgcattt ggcctatgta atcctgccca tggtggccgc 2880 agctaatcag aatcagatgg aaaattaaac cgggtaatct acttctaagc cttaagaata 2940 ttccctggga cacagacact ataattggaa gtgctgagct ctggggcaga aggatcaggt 3000 gaccttcgca acaaagtttg cccccacctc acataggacc cggaagcagc ctgagctgtg 3060 gcggaggatc caggaagcta cggagagaag cagccagcat ggtgttccgt gcctcccgga 3120 cgtttttcag gaggcctggt tggacttggg ttcctggatg gtgggattgt tgtacagcct 3180 ctcaggagac cctgctgtca agactgtgtg tgtggatttc tcacccttag aagctctact 3240 aagacatcaa cggaattagg gccttccttt ttgccttgtg agcgccaagg aaaagaaact 3300 atctcggtca cgtgagcgcc agcgaaaaga aactgtatca gtcatccaga gaccgtttat 3360 tgcccaacac gttattcttg ctgttggtgg ggtaactagc cgaggaagac acagcgcctt 3420 cccttcagga gttgcgtctc ctctgcaggc cacgatggtc tgctctggag cattgggtga 3480 acacacaggc tggctgctct gggcagcgcc ttcactctga ccctggagaa ccatttcatt 3540 tcatcctggt cagtctagag tctgtgcacc aggcagtcca tccactgaag gctgtgttta 3600 ttcttttcct gtgcccctca taaatggaag aaagtaaact gcttatcccg agccttaaaa 3660 aaa 3663 85 1344 DNA Homo sapiens misc_feature Incyte ID No 336615.1 85 ggaggaggag gcagctacgg tgataaagaa gagcaatcaa aagggcaaag ccaaaggaaa 60 aggcaaaaag aaagcgaagg aggagagggc cccgtctccc cccgtggagg tggacgaacc 120 ccgggagttt gtgctccggc ctgcccccca gggccgcacg gtgcgctgcc ggctgacccg 180 ggacaaaaag ggcatggatc gaggcatgta tccctcctac ttcctgcacc tggacacgga 240 gaagaaggtg ttcctcttgg ctggcaggaa acgaaaacgg agcaagacag ccaattacct 300 catctccatc gaccctacca atctgtcccg aggaggggag aatttcatcg ggaagctgag 360 gtccaacctc ctggggaacc gcttcacggt ctttgacaac gggcagaacc cacagcgtgg 420 gtacagcact aatgtggcaa gccttcggca ggagctggca gctgtgatct atgaaaccaa 480 cgtgctgggc ttccgtggcc cccggcgcat gaccgtcatc attcctggca tgagtgcgga 540 gaacgagagg gtccccatcc ggccccgaaa tgctagtgac ggcctgctgg tgcgctggca 600 gaacaagacg ctggagagcc tcatagaact gcacaacaag ccacctgtct ggaacgatga 660 cagtggctcc tacaccctca acttccaagg ccgggtcacc caggcctcag tcaagaactt 720 ccagattgtc cacgctgatg accccgacta tatcgtgctg cagttcggcc gcgtggcgga 780 ggacgccttc accctagact accggtaccc gctgtgcgcc ctgcaggcct tcgccatcgc 840 cctctccagt ttcgacggga agctggcctg cgagtgaccc cagcagcccc tcagcgcccc 900 cagagcccgt cagcgtgggg gaaaggattc agtggaggct ggcagggtcc ctccagcaaa 960 gctcccgcgg aaaactgctc ctgtgtcggg gctgacctct cactgcctct cggtgacctc 1020 cgtcctctcc ccagcctggc acaggccgag gcaggaggag cccggacggc gggtaggacg 1080 gagatgaaga acatctggag ttggagccgc acatctggtc tcggagctcg cctgcgccgc 1140 tgtgcccccc tcctccccgc gccccagtca cttcctgtcc gggagcagta gtcattgttg 1200 ttttaacctc ccctctcccc gggaccgcgc tagggctccg aggagctggg gcgggctagg 1260 aggagggggt aggtgatggg ggacgagggc caggcaccca catccccaat aaagccgcgt 1320 ccttgtgcaa aaaaaaaaaa aagg 1344 86 3156 DNA Homo sapiens misc_feature Incyte ID No 2733282CB1 86 gttcaggaag aaaccatctg catccatatt gaaaacctga cacaatgtat gcagcaggct 60 cagtgtgagt gaactggagg cttctctaca acatgaccca aaggagcatt gcaggtccta 120 tttgcaacct gaagtttgtg actctcctgg ttgccttaag ttcagaactc ccattcctgg 180 gagctggagt acagcttcaa gacaatgggt ataatggatt gctcattgca attaatcctc 240 aggtacctga gaatcagaac ctcatctcaa acattaagga aatgataact gaagcttcat 300 tttacctatt taatgctacc aagagaagag tatttttcag aaatataaag attttaatac 360 ctgccacatg gaaagctaat aataacagca aaataaaaca agaatcatat gaaaaggcaa 420 atgtcatagt gactgactgg tatggggcac atggagatga tccatacacc ctacaataca 480 gagggtgtgg aaaagaggga aaatacattc atttcacacc taatttccta ctgaatgata 540 acttaacagc tggctacgga tcacgaggcc gagtgtttgt ccatgaatgg gcccacctcc 600 gttggggtgt gttcgatgag tataacaatg acaaaccttt ctacataaat gggcaaaatc 660 aaattaaagt gacaaggtgt tcatctgaca tcacaggcat ttttgtgtgt gaaaaaggtc 720 cttgccccca agaaaactgt attattagta agctttttaa agaaggatgc acctttatct 780 acaatagcac ccaaaatgca actgcatcaa taatgttcat gcaaagttat ctctgtggtg 840 aaatttgtaa tgccagtacc cacaaccaag aagcaccaaa cctacagaac cagatgtgca 900 gcctcagaag tgcatgggat gtaatcacag actctgctga ctttcaccac agctttccca 960 tgaacgggac tgagcttcca cctcctccca cattctcgct tgtagaggct ggtgacaaag 1020 tggtctgttt agtgctggat gtgtccagca agatggcaga ggctgacaga ctccttcaac 1080 tacaacaagc cgcagaattt tatttgatgc agattgttga aattcatacc ttcgtgggca 1140 ttgccagttt cgacagcaaa ggagagatca gagcccagct acaccaaatt aacagcaatg 1200 atgatcgaaa gttgctggtt tcatatctgc ccaccactgt atcagctaaa acagacatca 1260 gcatttgttc agggcttaag aaaggatttg aggtggttga aaaactgaat ggaaaagctt 1320 atggctctgt gatgatatta gtgaccagcg gagatgataa gcttcttggc aattgcttac 1380 ccactgtgct cagcagtggt tcaacaattc actccattgc cctgggttca tctgcagccc 1440 caaatctgga ggaattatca cgtcttacag gaggtttaaa gttctttgtt ccagatatat 1500 caaactccaa tagcatgatt gatgctttca gtagaatttc ctctggaact ggagacattt 1560 tccagcaaca tattcagctt gaaagtacag gtgaaaatgt caaacctcac catcaattga 1620 aaaacacagt gactgtggat aatactgtgg gcaacgacac tatgtttcta gttacgtggc 1680 aggccagtgg tcctcctgag attatattat ttgatcctga tggacgaaaa tactacacaa 1740 ataattttat caccaatcta acttttcgga cagctagtct ttggattcca ggaacagcta 1800 agcctgggca ctggacttac accctgaaca atacccatca ttctctgcaa gccctgaaag 1860 tgacagtgac ctctcgcgcc tccaactcag ctgtgccccc agccactgtg gaagcctttg 1920 tggaaagaga cagcctccat tttcctcatc ctgtgatgat ttatgccaat gtgaaacagg 1980 gattttatcc cattcttaat gccactgtca ctgccacagt tgagccagag actggagatc 2040 ctgttacgct gagactcctt gatgatggag caggtgctga tgttataaaa aatgatggaa 2100 tttactcgag gtattttttc tcctttgctg caaatggtag atatagcttg aaagtgcatg 2160 tcaatcactc tcccagcata agcaccccag cccactctat tccagggagt catgctatgt 2220 atgtaccagg ttacacagca aacggtaata ttcagatgaa tgctccaagg aaatcagtag 2280 gcagaaatga ggaggagcga aagtggggct ttagccgagt cagctcagga ggctcctttt 2340 cagtgctggg agttccagct ggcccccacc ctgatgtgtt tccaccatgc aaaattattg 2400 acctggaagc tgtaaaagta gaagaggaat tgaccctatc ttggacagca cctggagaag 2460 actttgatca gggccaggct acaagctatg aaataagaat gagtaaaagt ctacagaata 2520 tccaagatga ctttaacaat gctattttag taaatacatc aaagcgaaat cctcagcaag 2580 ctggcatcag ggagatattt acgttctcac cccaaatttc cacgaatgga cctgaacatc 2640 agccaaatgg agaaacacat gaaagccaca gaatttatgt tgcaatacga gcaatggata 2700 ggaactcctt acagtctgct gtatctaaca ttgcccaggc gcctctgttt attcccccca 2760 attctgatcc tgtacctgcc agagattatc ttatattgaa aggagtttta acagcaatgg 2820 gtttgatagg aatcatttgc cttattatag ttgtgacaca tcatacttta agcaggaaaa 2880 agagagcaga caagaaagag aatggaacaa aattattata aataaatatc caaagtgtct 2940 tccttcttag atataagacc catggccttc gactacaaaa acatactaac aaagtcaaat 3000 taacatcaaa actgtattaa aatgcattga gtttttgtac aatacagata agatttttac 3060 atggtagatc aacaaattct ttttgggggt agattagaaa acccttacac tttggctatg 3120 aacaaataat aaaaattatt ctttaaaaaa aaaaaa 3156 87 942 PRT Homo sapiens misc_feature Incyte ID No 2733282CD1 87 Met Thr Gln Arg Ser Ile Ala Gly Pro Ile Cys Asn Leu Lys Phe 1 5 10 15 Val Thr Leu Leu Val Ala Leu Ser Ser Glu Leu Pro Phe Leu Gly 20 25 30 Ala Gly Val Gln Leu Gln Asp Asn Gly Tyr Asn Gly Leu Leu Ile 35 40 45 Ala Ile Asn Pro Gln Val Pro Glu Asn Gln Asn Leu Ile Ser Asn 50 55 60 Ile Lys Glu Met Ile Thr Glu Ala Ser Phe Tyr Leu Phe Asn Ala 65 70 75 Thr Lys Arg Arg Val Phe Phe Arg Asn Ile Lys Ile Leu Ile Pro 80 85 90 Ala Thr Trp Lys Ala Asn Asn Asn Ser Lys Ile Lys Gln Glu Ser 95 100 105 Tyr Glu Lys Ala Asn Val Ile Val Thr Asp Trp Tyr Gly Ala His 110 115 120 Gly Asp Asp Pro Tyr Thr Leu Gln Tyr Arg Gly Cys Gly Lys Glu 125 130 135 Gly Lys Tyr Ile His Phe Thr Pro Asn Phe Leu Leu Asn Asp Asn 140 145 150 Leu Thr Ala Gly Tyr Gly Ser Arg Gly Arg Val Phe Val His Glu 155 160 165 Trp Ala His Leu Arg Trp Gly Val Phe Asp Glu Tyr Asn Asn Asp 170 175 180 Lys Pro Phe Tyr Ile Asn Gly Gln Asn Gln Ile Lys Val Thr Arg 185 190 195 Cys Ser Ser Asp Ile Thr Gly Ile Phe Val Cys Glu Lys Gly Pro 200 205 210 Cys Pro Gln Glu Asn Cys Ile Ile Ser Lys Leu Phe Lys Glu Gly 215 220 225 Cys Thr Phe Ile Tyr Asn Ser Thr Gln Asn Ala Thr Ala Ser Ile 230 235 240 Met Phe Met Gln Ser Tyr Leu Cys Gly Glu Ile Cys Asn Ala Ser 245 250 255 Thr His Asn Gln Glu Ala Pro Asn Leu Gln Asn Gln Met Cys Ser 260 265 270 Leu Arg Ser Ala Trp Asp Val Ile Thr Asp Ser Ala Asp Phe His 275 280 285 His Ser Phe Pro Met Asn Gly Thr Glu Leu Pro Pro Pro Pro Thr 290 295 300 Phe Ser Leu Val Glu Ala Gly Asp Lys Val Val Cys Leu Val Leu 305 310 315 Asp Val Ser Ser Lys Met Ala Glu Ala Asp Arg Leu Leu Gln Leu 320 325 330 Gln Gln Ala Ala Glu Phe Tyr Leu Met Gln Ile Val Glu Ile His 335 340 345 Thr Phe Val Gly Ile Ala Ser Phe Asp Ser Lys Gly Glu Ile Arg 350 355 360 Ala Gln Leu His Gln Ile Asn Ser Asn Asp Asp Arg Lys Leu Leu 365 370 375 Val Ser Tyr Leu Pro Thr Thr Val Ser Ala Lys Thr Asp Ile Ser 380 385 390 Ile Cys Ser Gly Leu Lys Lys Gly Phe Glu Val Val Glu Lys Leu 395 400 405 Asn Gly Lys Ala Tyr Gly Ser Val Met Ile Leu Val Thr Ser Gly 410 415 420 Asp Asp Lys Leu Leu Gly Asn Cys Leu Pro Thr Val Leu Ser Ser 425 430 435 Gly Ser Thr Ile His Ser Ile Ala Leu Gly Ser Ser Ala Ala Pro 440 445 450 Asn Leu Glu Glu Leu Ser Arg Leu Thr Gly Gly Leu Lys Phe Phe 455 460 465 Val Pro Asp Ile Ser Asn Ser Asn Ser Met Ile Asp Ala Phe Ser 470 475 480 Arg Ile Ser Ser Gly Thr Gly Asp Ile Phe Gln Gln His Ile Gln 485 490 495 Leu Glu Ser Thr Gly Glu Asn Val Lys Pro His His Gln Leu Lys 500 505 510 Asn Thr Val Thr Val Asp Asn Thr Val Gly Asn Asp Thr Met Phe 515 520 525 Leu Val Thr Trp Gln Ala Ser Gly Pro Pro Glu Ile Ile Leu Phe 530 535 540 Asp Pro Asp Gly Arg Lys Tyr Tyr Thr Asn Asn Phe Ile Thr Asn 545 550 555 Leu Thr Phe Arg Thr Ala Ser Leu Trp Ile Pro Gly Thr Ala Lys 560 565 570 Pro Gly His Trp Thr Tyr Thr Leu Asn Asn Thr His His Ser Leu 575 580 585 Gln Ala Leu Lys Val Thr Val Thr Ser Arg Ala Ser Asn Ser Ala 590 595 600 Val Pro Pro Ala Thr Val Glu Ala Phe Val Glu Arg Asp Ser Leu 605 610 615 His Phe Pro His Pro Val Met Ile Tyr Ala Asn Val Lys Gln Gly 620 625 630 Phe Tyr Pro Ile Leu Asn Ala Thr Val Thr Ala Thr Val Glu Pro 635 640 645 Glu Thr Gly Asp Pro Val Thr Leu Arg Leu Leu Asp Asp Gly Ala 650 655 660 Gly Ala Asp Val Ile Lys Asn Asp Gly Ile Tyr Ser Arg Tyr Phe 665 670 675 Phe Ser Phe Ala Ala Asn Gly Arg Tyr Ser Leu Lys Val His Val 680 685 690 Asn His Ser Pro Ser Ile Ser Thr Pro Ala His Ser Ile Pro Gly 695 700 705 Ser His Ala Met Tyr Val Pro Gly Tyr Thr Ala Asn Gly Asn Ile 710 715 720 Gln Met Asn Ala Pro Arg Lys Ser Val Gly Arg Asn Glu Glu Glu 725 730 735 Arg Lys Trp Gly Phe Ser Arg Val Ser Ser Gly Gly Ser Phe Ser 740 745 750 Val Leu Gly Val Pro Ala Gly Pro His Pro Asp Val Phe Pro Pro 755 760 765 Cys Lys Ile Ile Asp Leu Glu Ala Val Lys Val Glu Glu Glu Leu 770 775 780 Thr Leu Ser Trp Thr Ala Pro Gly Glu Asp Phe Asp Gln Gly Gln 785 790 795 Ala Thr Ser Tyr Glu Ile Arg Met Ser Lys Ser Leu Gln Asn Ile 800 805 810 Gln Asp Asp Phe Asn Asn Ala Ile Leu Val Asn Thr Ser Lys Arg 815 820 825 Asn Pro Gln Gln Ala Gly Ile Arg Glu Ile Phe Thr Phe Ser Pro 830 835 840 Gln Ile Ser Thr Asn Gly Pro Glu His Gln Pro Asn Gly Glu Thr 845 850 855 His Glu Ser His Arg Ile Tyr Val Ala Ile Arg Ala Met Asp Arg 860 865 870 Asn Ser Leu Gln Ser Ala Val Ser Asn Ile Ala Gln Ala Pro Leu 875 880 885 Phe Ile Pro Pro Asn Ser Asp Pro Val Pro Ala Arg Asp Tyr Leu 890 895 900 Ile Leu Lys Gly Val Leu Thr Ala Met Gly Leu Ile Gly Ile Ile 905 910 915 Cys Leu Ile Ile Val Val Thr His His Thr Leu Ser Arg Lys Lys 920 925 930 Arg Ala Asp Lys Lys Glu Asn Gly Thr Lys Leu Leu 935 940 88 1121 DNA Homo sapiens misc_feature Incyte ID No 399161.1 88 caggcgggag caccgtgcct ggcccagatg gatttttaaa tatcacctgt tcatattgtt 60 taaaatagat acaactaaaa cagctttgag gcatacagga actctacaga taaggaggac 120 catttcataa tgataaaggg cttatctcac caagaaggca gtcacactta cgtttttatg 180 tatttgttga agagtcccaa tgtatttaaa gcaaaaataa gcaactacaa agagaaagat 240 acaaatccat gatcaaagtg aggaattttc acacacatcg tagtaactga tggaatgagt 300 caatgaaaaa ttagtgagga aatagaagat ttggacagca caacaaatgg cctaggagaa 360 catttagaat gttgccttcg atgcttaaga atacatattc ttttcaaaag aaaacccaga 420 acagcctggc aggagagata ccatcatcat gaaggtgatt ttcccagagc tgggcttatc 480 cattgcattc tggatgtgct gacgcctgtg gttttcccaa atgtgggaaa ctggactgca 540 taatttgtgg tagtggggga ctatgttcgt gttctctcct ggtgtttaaa attaaaaaaa 600 aaaaaacttt attaaaggca cagaacatta ataaaaattg acaataaact gggctattaa 660 gtaaattgca acaatttcca gaggtttgaa atgatacaga gtatgttttc tgaccacagt 720 acagttaaac taggaatata acaaaaagat aactagggat atgtgtggat attgcatacc 780 tctaagtaac ccttgggatg agaaagaaat tacaatggaa attagaaaat atcttgaata 840 atgaaaatac aatatatgta agcttgtaga attcagctta ttaaatgcat attttagaaa 900 gaaggaaagg ctgaaaatca gtgagcaaag ccttccatct caagaaatag aaaaagaata 960 tagaaggaag gaattaatat ttttaaagaa gcactaattt acaagaataa ttaaatagaa 1020 aagaagttgt cattaggaag gatcaataaa gctagaagct tgttatttgn aaagacttgt 1080 aaatgtggta aatcacaagt aacgtacgta gatgaaaagg g 1121 89 721 DNA Homo sapiens misc_feature Incyte ID No 339638.1 89 gtggcccaca gcgaactaga gaaacaaaag gagagtcttt taccccctgg agttatcgcc 60 atcagcaaac tgagagctgc ctctcttcct ctccctgccc tgtgtctgtc tccacctcct 120 tccctctcat ccttgctctt tcccttttct ctttatcccc cgcccccttt ctttctcttc 180 ctcctttctc ctcccaggga ccaaagggag aagggagagc cgagaaagtg gccctgccat 240 cccctactgg aataaccgcc gccgcngccc catcactggt ggccacatcc cttctaattt 300 gtagtggtgg gtttctttcc ttgaagagca gggtactttt aaacagatag aggtaatggg 360 aggattaata ttcataggta agtccaaacg gaaaatgttt agcttcctta caccaaaggt 420 ctgctgtgtc tgagattaca ctaagttcaa gcaacatcat gtcagtgaag aagccattag 480 ctgcaggaac acactgagaa gtgagggagc ctgtctacca gaaggaaatg gagctaggat 540 ctttgcaaac tgctgagtag agaggagagg acgagtaaat gagacagacg gaaaagagct 600 ggaagagaga gactccttta tggcacattt ttatcctgag atttccaagc attttatata 660 tattgcatgg taaagaggaa ttgaaatagc caaaagaaat gaactaaaat gaaaagggag 720 g 721 90 538 DNA Homo sapiens misc_feature Incyte ID No 697785CB1 90 cccacgcgtc cggtggagtc ttctgacagc tggtgcgcct gcccgggaac atcctcctgg 60 actcaatcat ggcttgtggt ctggtcgcca gcaacctgaa tctcaaacct ggagagtgcc 120 ttcgagtgcg aggcgaggtg gctcctgacg ctaagagctt cgtgctgaac ctgggcaaag 180 acagcaacaa cctgtgcctg cacttcaacc ctcgcttcaa cgcccacggc gacgccaaca 240 ccatcgtgtg caacagcaag gacggcgggg cctgggggac cgagcagcgg gaggctgtct 300 ttcccttcca gcctggaagt gttgcagagg tgtgcatcac cttcgaccag gccaacctga 360 ccgtcaagct gccagatgga tacgaattca agttccccaa ccgcctcaac ctggaggcca 420 tcaactacat ggcagctgac ggtgacttca agatcaaatg tgtggccttt gactgaaatc 480 agccagccca tggcccccaa taaaggcagc tgcctctgct ccctctgaaa aaaaaaaa 538 91 135 PRT Homo sapiens misc_feature Incyte ID No 697785CD1 91 Met Ala Cys Gly Leu Val Ala Ser Asn Leu Asn Leu Lys Pro Gly 1 5 10 15 Glu Cys Leu Arg Val Arg Gly Glu Val Ala Pro Asp Ala Lys Ser 20 25 30 Phe Val Leu Asn Leu Gly Lys Asp Ser Asn Asn Leu Cys Leu His 35 40 45 Phe Asn Pro Arg Phe Asn Ala His Gly Asp Ala Asn Thr Ile Val 50 55 60 Cys Asn Ser Lys Asp Gly Gly Ala Trp Gly Thr Glu Gln Arg Glu 65 70 75 Ala Val Phe Pro Phe Gln Pro Gly Ser Val Ala Glu Val Cys Ile 80 85 90 Thr Phe Asp Gln Ala Asn Leu Thr Val Lys Leu Pro Asp Gly Tyr 95 100 105 Glu Phe Lys Phe Pro Asn Arg Leu Asn Leu Glu Ala Ile Asn Tyr 110 115 120 Met Ala Ala Asp Gly Asp Phe Lys Ile Lys Cys Val Ala Phe Asp 125 130 135 92 866 DNA Homo sapiens misc_feature Incyte ID No 399785.1 92 acgagacgag cacccgtngg gggctggagc accccgcgcg ctcccctggc gagagggagg 60 gtcgtggctc ggcccctgct cagacaaagg ctgggaggcg ggagacatgc acttcccctt 120 ccttttcagc caggcgcgcg ctgataccag gcccacgtca gctatttttg gagcctttta 180 cacgacagct ggaggagcgt cctttttaat tttccccttt tgtttggccg cccccacccc 240 caccccttcg ccttcatcgc tgcacttgag gctccatcct ggggcctctc cttgacttga 300 cctgccttgg caggcacatg ccctccctgc ctggctcact cgccgcagag acctggcagc 360 ccgcgcaaaa tgtcactttg cggaatcgtt cccacggctt ctgggtaccc ttagttccct 420 gcttagggag ggaagacagt agtcgggtcg taataagcaa gacttagccc gagcctccgt 480 tgccaacgca ggctgccttg cttggcgtgt gggcatcggc ctgccccctc accctggcta 540 cccaacacag ctacaaaagg cagggaacaa tgtaggtccc ttggccctgc ctaatgcctg 600 ttgccatgga aacccctatc ctaatctggc caggagcccc ttgcagtgag ccaggagagt 660 gaggaagagg ggatggggcc cgctggcctg aacctggcca gaggaggtaa tggttaaccg 720 gattgtggga gcagctgact agagccgggg gggtagggag gcttgggccc cagtcctacc 780 ttccctgcca aggagaaagg ggcatgtctg cttttgtacc tctgggaatc tacctcaggg 840 atctgcccaa caactcccag gttcca 866 93 1274 DNA Homo sapiens misc_feature Incyte ID No 002455.1 93 gcggccgcca gcttgcaaag ccgaagtctg gccgcgctct tcgactcgct gcgccacgtc 60 cccgggggtg ccgagccggc ggggggtgag tggtctgcgc cggcggccgc gctaggaggt 120 gcgggcactt gggggcgccg ggaaggggaa cttggcagcc ccgcgggggc cacgggcgat 180 cccaggggcc aggaaggtcc cgctgcgggc acgcaatctg cctccgtcct tcttcacgga 240 gccgtcccgg gcaggcggcg gcgggtgtgg cccgtcgggg ccggacgtga gcttgggcga 300 cctggagaag ggcgcggagg ccgtggagtt ctttgagctg ctggggcccg actacggcgc 360 cggcacggag gcggcagtct tgcttgccgc cgagcctctc gacgtgttcc ccgccggagc 420 ctccgtactg cggggacccc cggagctgga gcccggcctc tttgagccgc cgccggcagt 480 ggtgggaaac ctactgtacc ccgagccctg gagcgtcccg ggctgctccc cgaccaaaaa 540 gagccccctg actgcccccc gcggcggctt gaccttgaac gagcccttga gccccctgta 600 ccccgccgct gcggattctc ccggcgggga ggacgggcgg ggccatttgg cctctttcgc 660 ccccttcttt ccagactgcg ccctgccccc gacgccgccg ccccatcagg tgtcctacga 720 ttacagcgcg ggctacagcc gcaccgccta ttccagcctt tggagatccg acggggtttg 780 ggaaggggcg ccgggggagg agggggcgca ccgggactga cttcgaggca cgcttccctt 840 cattagagac ggctgtggag agcgccgcgc ctccgtgggt ttctcctaaa tctgaagaac 900 gatgggaaaa tgcacgtgga gatgaaacca gatttttaaa aattcaatta ataaaagcaa 960 cttcagaaaa aagagatgaa gacgagttgg ggattgttta atcacaacct caagtgttaa 1020 aacaaaaaca aacaaacacg tttgtaggtt cttactggac cagaggagtc aagaaaccaa 1080 gatggtttgg ggtatggggt ggggacggca aaaggggtaa gagctggctt ctgtagccac 1140 ctgtcccttc tatttttcag cgaaggtcag tgtatttagt gtaattaccc cttctaaaca 1200 gtgtcctagt ccctcccttc cctctccttg agtgcatttt gaattaaagc ctatattgaa 1260 aaaaaaaaaa aagg 1274 94 924 DNA Homo sapiens misc_feature Incyte ID No 1382920.38 94 atctagaact accgagagtc gtcggggttt cctgcttcaa cagtgcttgg acggaacccg 60 gcgctcgttc cccaccccgg ccggccgccc atagccagcc ctccgtcacc tcttcaccgc 120 accctcggac tgccccaagg cccccgccgc cgctccagcg ccgcgcagcc accgccgccg 180 ccgcctcctt tccttagtcg ccgccatgac gaccgcgtcc acctgcgcag gtgccgccag 240 aactaccacc aggactcaga ggccgccatc aaccgccaga tcaacctgga gctctacgcc 300 tcctacgttt acctgtccat gtcttactac tttgaccgcg atgatgtggc tttgaagaac 360 tttgccaaat actttcttca ccaatctcat gaggagaggg aacatgctga gaaactgatg 420 aagctgcaga accaacgagg tggccgaatc ttccttcagg atatcaagaa accagactgt 480 gatgactggg agagcgggct gaatgcaatg gagtgtgcat tacatttgga aaaaaatgtg 540 aatcagtcac tactggaact gcacaaactg gccactgaca aaaatgaccc ccatttgtgt 600 gacttcattg agacacatta cctgaatgag caggtgaaag ccatcaaaga attgggtgac 660 cacgtgacca acttgcgcaa gatgggagcg cccgaatctg gcttggcgga atatctcttt 720 gacaagcaca ccctgggaga cagtgataat gaaagctaag cctcgggcta atttccccat 780 agccgtgggg tgactttcct ggtcaccaag gcagtgcatg catgttgggg tttcctttac 840 cttttctata agttgtacca aaacatccac ttaagttctt tgatttgtac cattccttca 900 aataaagaaa tttggtaccc aaaa 924 95 634 DNA Homo sapiens misc_feature Incyte ID No 334749.1 95 gacgcccatc aatgaacaaa caagattccc actgtcccat ctcctatcca gtgaaacaca 60 gccaacttga taatttgtgc agggaaagac tctgtttagc ttataccttg aacctaaggg 120 aaattaaatt gcacattttc tgttcctggc taatcttctg aataatgtac tgaacacagt 180 aggagttaag aattaaaaat acctgtctgc agtttcagaa acaatcacac acaaaatatt 240 tgtttatttc cagactgatg aaagactgaa tttttggtct catgtattta ctgtattgtt 300 tcatatattt atctatatgc tttggctgta ttaacttgtt gaaatagttt gtggttcttt 360 atatttagct tttataaata attgaaaatc taatgaatgc ttacttaata accaatctaa 420 actggggact tcaaacatag ggagtcaagt aatctggttg tgtaataaat aagcaagttg 480 ttatctttca ggctgagggc atatcaacca agctaaaaga cgtgtgtgta ttaaaaaaaa 540 aaaaaagtct accaaaccac catatgatat ccaaggttaa ctatatagga ggtctaataa 600 cattcagaag gtgctagatg aatataccaa aaac 634 96 579 DNA Homo sapiens misc_feature Incyte ID No 041764.1 96 gaaaaaccat ataatggagg aaggccttgc cccaaactgg accatgtcaa ccaggcacag 60 gtgtatgagg ttgtcccatg ccacagtgac tgcaaccagt acctatgggt cacagagccc 120 tggagcatct gcaaggtgac ctttgtgaat atgcgggaga actgtggaga gggcgtgcaa 180 acccgaaaag tgagatgcat gcagaataca gcagatggcc cttctgaaca tgtagaggat 240 tacctctgtg acccagaaga gatgcccctg ggctctagag tgtgcaaatt accatgccct 300 gaggactgtg tgatatctga atggggtcca tggacccaat gtgttttgcc ttgcaatcaa 360 agcagtttcc ggcaaaggtc agctgatccc atcagacaac cagctgatga aggaagatct 420 tgccctaatg ctgttgagaa agaaccctgt aacctgaaca aaaactgcta ccactatgat 480 tataatgtaa cagactggag tacatgtcag ctgagtgaga aggcagtttg tggaaatgga 540 ataaaaacaa ggatgttgga ttgtgttcga agtgatggc 579 97 10432 DNA Homo sapiens misc_feature Incyte ID No 2700132CB1 97 tggttcgaca agtggccttg cgggccggat cgtcccagtg gaagagttgt aaatttgctt 60 ctggccttcc cctacggatt atacctggcc ttcccctacg gattatactc aacttactgt 120 ttagaaaatg tggcccacga gacgcctggt tactatcaaa aggagcgggg tcgacggtcc 180 ccactttccc ctgagcctca gcacctgctt gtttggaagg ggtattgaat gtgacatccg 240 tatccagctt cctgttgtgt caaaacaaca ttgcaaaatt gaaatccatg agcaggaggc 300 aatattacat aatttcagtt ccacaaatcc aacacaagta aatgggtctg ttattgatga 360 gcctgtacgg ctaaaacatg gagatgtaat aactattatt gatcgttcct tcaggtatga 420 aaatgaaagt cttcagagtg gaaggaagtc aactgaattt ccaagaaaaa tacgtgaaca 480 ggagccagca cgtcgtgtct caagatctag cttctcttct gaccctgatg agaaagctca 540 agattccaag gcctattcaa aaatcactga aggaaaagtt tcaggaaatc ctcaggtaca 600 tatcaagaat gtcaaagaag acagtaccgc agatgactca aaagacagtg ttgctcaggg 660 aacaactaat gttcattcct cagaacatgc tggacgtaat ggcagaaatg cagctgatcc 720 catttctggg gattttaaag aaatttccag cgttaaatta gtgagccgtt atggagaatt 780 gaagtctgtt cccactacac aatgtcttga caatagcaaa aaaaatgaat ctcccttttg 840 gaagctttat gagtcagtga agaaagagtt ggatgtaaaa tcacaaaaag aaaatgtcct 900 acagtattgt agaaaatctg gattacaaac tgattacgca acagagaaag aaagtgctga 960 tggtttacag ggggagaccc aactgttggt ctcgcgtaag tcaagaccaa aatctggtgg 1020 gagcggccac gctgtggcag agcctgcttc acctgaacaa gagcttgacc agaacaaggg 1080 gaagggaaga gacgtggagt ctgttcagac tcccagcaag gctgtgggcg ccagctttcc 1140 tctctatgag ccggctaaaa tgaagacccc tgtacaatat tcacagcaac aaaattctcc 1200 acaaaaacat aagaacaaag acctgtatac tactggtaga agagaatctg tgaatctggg 1260 taaaagtgaa ggcttcaagg ctggtgataa aactcttact cccaggaagc tttcaactag 1320 aaatcgaaca ccagctaaag ttgaagatgc agctgactct gccactaagc cagaaaatct 1380 ctcttccaaa accagaggaa gtattcctac agatgtggaa gttctgccta cggaaactga 1440 aattcacaat gagccatttt taactctgtg gctcactcaa gttgagagga agatccaaaa 1500 ggattccctc agcaagcctg agaaattggg cactacagct ggacagatgt gctctgggtt 1560 acctggtctt agttcagttg atatcaacaa ctttggtgat tccattaatg agagtgaggg 1620 aatacctttg aaaagaaggc gtgtgtcctt tggtgggcac ctaagacctg aactatttga 1680 tgaaaacttg cctcctaata cgcctctcaa aaggggagaa gccccaacca aaagaaagtc 1740 tctggtaatg cacactccac ctgtcctgaa gaaaatcatc aaggaacagc ctcaaccatc 1800 aggaaaacaa gagtcaggtt cagaaatcca tgtggaagtg aaggcacaaa gcttggttat 1860 aagccctcca gctcctagtc ctaggaaaac tccagttgcc agtgatcaac gccgtaggtc 1920 ctgcaaaaca gcccctgctt ccagcagcaa atctcagaca gaggttccta agagaggagg 1980 agaaagagtg gcaacctgcc ttcaaaagag agtgtctatc agccgaagtc aacatgatat 2040 tttacagatg atatgttcca aaagaagaag tggtgcttcg gaagcaaatc tgattgttgc 2100 aaaatcatgg gcagatgtag taaaacttgg tgcaaaacaa acacaaacta aagtcataaa 2160 acatggtcct caaaggtcaa tgaacaaaag gcaaagaaga cctgctactc caaagaagcc 2220 tgtgggcgaa gttcacagtc aatttagtac aggccacgca aactctcctt gtaccataat 2280 aatagggaaa gctcatactg aaaaagtaca tgtgcctgct cgaccctaca gagtgctcaa 2340 caacttcatt tccaaccaaa aaatggactt taaggaagat ctttcaggaa tagctgaaat 2400 gttcaagacc ccagtgaagg agcaaccgca gttgacaagc acatgtcaca tcgctatttc 2460 aaattcagag aatttgcttg gaaaacagtt tcaaggaact gattcaggag aagaacctct 2520 gctccccacc tcagagagtt ttggaggaaa tgtgttcttc agtgcacaga atgcagcaaa 2580 acagccatct gataaatgct ctgcaagccc tcccttaaga cggcagtgta ttagagaaaa 2640 tggaaacgta gcaaaaacgc ccaggaacac ctacaaaatg acttctctgg agacaaaaac 2700 ttcagatact gagacagagc cttcaaaaac agtatccact gtaaacaggt caggaaggtc 2760 tacagagttc aggaatatac agaagctacc tgtggaaagt aagagtgaag aaacaaatac 2820 agaaattgtt gagtgcatcc taaaaagagg tcagaaggca acactactac aacaaaggag 2880 agaaggagag atgaaggaaa tagaaagacc ttttgagaca tataaggaaa atattgaatt 2940 aaaagaaaac gatgaaaaga tgaaagcaat gaagagatca agaacttggg ggcagaaatg 3000 tgcaccaatg tctgacctga cagacctcaa gagcttgcct gatacagaac tcatgaaaga 3060 cacggcacgt ggccagaatc tcctccaaac ccaagatcat gccaaggcac caaagagtga 3120 gaaaggcaaa atcactaaaa tgccctgcca gtcattacaa ccagaaccaa taaacacccc 3180 aacacacaca aaacaacagt tgaaggcatc cctggggaaa gtaggtgtga aagaagagct 3240 cctagcagtc ggcaagttca cacggacgtc aggggagacc acgcacacgc acagagagcc 3300 agcaggagat ggcaagagca tcagaacgtt taaggagtct ccaaagcaga tcctggaccc 3360 agcagcccgt gtaactggaa tgaagaagtg gccaagaacg cctaaggaag aggcccagtc 3420 actagaagac ctggctggct tcaaagagct cttccagaca ccaggtccct ctgaggaatc 3480 aatgactgat gagaaaacta ccaaaatagc ctgcaaatct ccaccaccag aatcagtgga 3540 cactccaaca agcacaaagc aatggcctaa gagaagtctc aggaaagcag atgtagagga 3600 agaattctta gcactcagga aactaacacc atcagcaggg aaagccatgc ttacgcccaa 3660 accagcagga ggtgatgaga aagacattaa agcatttatg ggaactccag tgcagaaact 3720 ggacctggca ggaactttac ctggcagcaa aagacagcta cagactccta aggaaaaggc 3780 ccaggctcta gaagacctgg ctggctttaa agagctcttc cagactcctg gtcacaccga 3840 ggaattagtg gctgctggta aaaccactaa aataccctgc gactctccac agtcagaccc 3900 agtggacacc ccaacaagca caaagcaacg acccaagaga agtatcagga aagcagatgt 3960 agagggagaa ctcttagcgt gcaggaatct aatgccatca gcaggcaaag ccatgcacac 4020 gcctaaacca tcagtaggtg aagagaaaga catcatcata tttgtgggaa ctccagtgca 4080 gaaactggac ctgacagaga acttaaccgg cagcaagaga cggccacaaa ctcctaagga 4140 agaggcccag gctctggaag acctgactgg ctttaaagag ctcttccaga cccctggtca 4200 tactgaagaa gcagtggctg ctggcaaaac tactaaaatg ccctgcgaat cttctccacc 4260 agaatcagca gacaccccaa caagcacaag aaggcagccc aagacacctt tggagaaaag 4320 ggacgtacag aaggagctct cagccctgaa gaagctcaca cagacatcag gggaaaccac 4380 acacacagat aaagtaccag gaggtgagga taaaagcatc aacgcgttta gggaaactgc 4440 aaaacagaaa ctggacccag cagcaagtgt aactggtagc aagaggcacc caaaaactaa 4500 ggaaaaggcc caacccctag aagacctggc tggctggaaa gagctcttcc agacaccagt 4560 atgcactgac aagcccacga ctcacgagaa aactaccaaa atagcctgca gatcacaacc 4620 agacccagtg gacacaccaa caagctccaa gccacagtcc aagagaagtc tcaggaaagt 4680 ggacgtagaa gaagaattct tcgcactcag gaaacgaaca ccatcagcag gcaaagccat 4740 gcacacaccc aaaccagcag taagtggtga gaaaaacatc tacgcattta tgggaactcc 4800 agtgcagaaa ctggacctga cagagaactt aactggcagc aagagacggc tacaaactcc 4860 taaggaaaag gcccaggctc tagaagacct ggctggcttt aaagagctct tccagacacg 4920 aggtcacact gaggaatcaa tgactaacga taaaactgcc aaagtagcct gcaaatcttc 4980 acaaccagac ctagacaaaa acccagcaag ctccaagcga cggctcaaga catccctggg 5040 gaaagtgggc gtgaaagaag agctcctagc agttggcaag ctcacacaga catcaggaga 5100 gactacacac acacacacag agccaacagg agatggtaag agcatgaaag catttatgga 5160 gtctccaaag cagatcttag actcagcagc aagtctaact ggcagcaaga ggcagctgag 5220 aactcctaag ggaaagtctg aagtccctga agacctggcc ggcttcatcg agctcttcca 5280 gacaccaagt cacactaagg aatcaatgac taatgaaaaa actaccaaag tatcctacag 5340 agcttcacag ccagacctag tggacacccc aacaagctcc aagccacagc ccaagagaag 5400 tctcaggaaa gcagacactg aagaagaatt tttagcattt aggaaacaaa cgccatcagc 5460 aggcaaagcc atgcacacac ccaaaccagc agtaggtgaa gagaaagaca tcaacacgtt 5520 tttgggaact ccagtgcaga aactggacca gccaggaaat ttacctggca gcaatagacg 5580 gctacaaact cgtaaggaaa aggcccaggc tctagaagaa ctgactggct tcagagagct 5640 tttccagaca ccatgcactg ataaccccac gactgatgag aaaactacca aaaaaatact 5700 ctgcaaatct ccgcaatcag acccagcgga caccccaaca aacacaaagc aacggcccaa 5760 gagaagcctc aagaaagcag acgtagagga agaattttta gcattcagga aactaacacc 5820 atcagcaggc aaagccatgc acacgcctaa agcagcagta ggtgaagaga aagacatcaa 5880 cacatttgtg gggactccag tggagaaact ggacctgcta ggaaatttac ctggcagcaa 5940 gagacggcca caaactccta aagaaaaggc caaggctcta gaagatctgg ctggcttcaa 6000 agagctcttc cagacaccag gtcacactga ggaatcaatg accgatgaca aaatcacaga 6060 agtatcctgc aaatctccac aaccagaccc agtcaaaacc ccaacaagct ccaagcaacg 6120 actcaagata tccttgggga aagtaggtgt gaaagaagag gtcctaccag tcggcaagct 6180 cacacagacg tcagggaaga ccacacagac acacagagag acagcaggag atggaaagag 6240 catcaaagcg tttaaggaat ctgcaaagca gatgctggac ccagcaaact atggaactgg 6300 gatggagagg tggccaagaa cacctaagga agaggcccaa tcactagaag acctggccgg 6360 cttcaaagag ctcttccaga caccagacca cactgaggaa tcaacaactg atgacaaaac 6420 taccaaaata gcctgcaaat ctccaccacc agaatcaatg gacactccaa caagcacaag 6480 gaggcggccc aaaacacctt tggggaaaag ggatatagtg gaagagctct cagccctgaa 6540 gcagctcaca cagaccacac acacagacaa agtaccagga gatgaggata aaggcatcaa 6600 cgtgttcagg gaaactgcaa aacagaaact ggacccagca gcaagtgtaa ctggtagcaa 6660 gaggcagcca agaactccta agggaaaagc ccaaccccta gaagacttgg ctggcttgaa 6720 agagctcttc cagacaccaa tatgcactga caagcccacg actcatgaga aaactaccaa 6780 aatagcctgc agatctccac aaccagaccc agtgggtacc ccaacaatct tcaagccaca 6840 gtccaagaga agtctcagga aagcagacgt agaggaagaa tccttagcac tcaggaaacg 6900 aacaccatca gtagggaaag ctatggacac acccaaacca gcaggaggtg atgagaaaga 6960 catgaaagca tttatgggaa ctccagtgca gaaattggac ctgccaggaa atttacctgg 7020 cagcaaaaga tggccacaaa ctcctaagga aaaggcccag gctctagaag acctggctgg 7080 cttcaaagag ctcttccaga caccaggcac tgacaagccc acgactgatg agaaaactac 7140 caaaatagcc tgcaaatctc cacaaccaga cccagtggac accccagcaa gcacaaagca 7200 acggcccaag agaaacctca ggaaagcaga cgtagaggaa gaatttttag cactcaggaa 7260 acgaacacca tcagcaggca aagccatgga cacaccaaaa ccagcagtaa gtgatgagaa 7320 aaatatcaac acatttgtgg aaactccagt gcagaaactg gacctgctag gaaatttacc 7380 tggcagcaag agacagccac agactcctaa ggaaaaggct gaggctctag aggacctggt 7440 tggcttcaaa gaactcttcc agacaccagg tcacactgag gaatcaatga ctgatgacaa 7500 aatcacagaa gtatcctgta aatctccaca gccagagtca ttcaaaacct caagaagctc 7560 caagcaaagg ctcaagatac ccctggtgaa agtggacatg aaagaagagc ccctagcagt 7620 cagcaagctc acacggacat caggggagac tacgcaaaca cacacagagc caacaggaga 7680 tagtaagagc atcaaagcgt ttaaggagtc tccaaagcag atcctggacc cagcagcaag 7740 tgtaactggt agcaggaggc agctgagaac tcgtaaggaa aaggcccgtg ctctagaaga 7800 cctggttgac ttcaaagagc tcttctcagc accaggtcac actgaagagt caatgactat 7860 tgacaaaaac acaaaaattc cctgcaaatc tcccccacca gaactaacag acactgccac 7920 gagcacaaag agatgcccca agacacgtct caggaaagaa gtaaaagagg agctctcagc 7980 agttgagagg ctcacgcaaa catcagggca aagcacacac acacacaaag aaccagcaag 8040 cggtgatgag ggcatcaaag tattgaagca acgtgcaaag aagaaaccaa acccagtaga 8100 agaggaaccc agcaggagaa ggccaagagc acctaaggaa aaggcccaac ccctggaaga 8160 cctggccggc ttcacagagc tctctgaaac atcaggtcac actcaggaat cactgactgc 8220 tggcaaagcc actaaaatac cctgcgaatc tcccccacta gaagtggtag acaccacagc 8280 aagcacaaag aggcatctca ggacacgtgt gcagaaggta caagtaaaag aagagccttc 8340 agcagtcaag ttcacacaaa catcagggga aaccacggat gcagacaaag aaccagcagg 8400 tgaagataaa ggcatcaaag cattgaagga atctgcaaaa cagacaccgg ctccagcagc 8460 aagtgtaact ggcagcagga gacggccaag agcacccagg gaaagtgccc aagccataga 8520 agacctagct ggcttcaaag acccagcagc aggtcacact gaagaatcaa tgactgatga 8580 caaaaccact aaaataccct gcaaatcatc accagaacta gaagacaccg caacaagctc 8640 aaagagacgg cccaggacac gtgcccagaa agtagaagtg aaggaggagc tgttagcagt 8700 tggcaagctc acacaaacct caggggagac cacgcacacc gacaaagagc cggtaggtga 8760 gggcaaaggc acgaaagcat ttaagcaacc tgcaaagcgg aagctggacg cagaagatgt 8820 aattggcagc aggagacagc caagagcacc taaggaaaag gcccaacccc tggaagatct 8880 ggccagcttc caagagctct ctcaaacacc aggccacact gaggaactgg caaatggtgc 8940 tgctgatagc tttacaagcg ctccaaagca aacacctgac agtggaaaac ctctaaaaat 9000 atccagaaga gttcttcggg cccctaaagt agaacccgtg ggagacgtgg taagcaccag 9060 agaccctgta aaatcacaaa gcaaaagcaa cacttccctg cccccactgc ccttcaagag 9120 gggaggtggc aaagatggaa gcgtcacggg aaccaagagg ctgcgctgca tgccagcacc 9180 agaggaaatt gtggaggagc tgccagccag caagaagcag agggttgctc ccagggcaag 9240 aggcaaatca tccgaacccg tggtcatcat gaagagaagt ttgaggactt ctgcaaaaag 9300 aattgaacct gcggaagagc tgaacagcaa cgacatgaaa accaacaaag aggaacacaa 9360 attacaagac tcagtccctg aaaataaggg aatatccctg cgctccagac gccaaaataa 9420 gactgaggca gaacagcaaa taactgaggt ctttgtatta gcagaaagaa tagaaataaa 9480 cagaaatgaa aagaagccca tgaagacctc cccagagatg gacattcaga atccagatga 9540 tggagcccgg aaacccatac ctagagacaa agtcactgag aacaaaaggt gcttgaggtc 9600 tgctagacag aatgagagct cccagcctaa ggtggcagag gagagcggag ggcagaagag 9660 tgcgaaggtt ctcatgcaga atcagaaagg gaaaggagaa gcaggaaatt cagactccat 9720 gtgcctgaga tcaagaaaga caaaaagcca gcctgcagca agcactttgg agagcaaatc 9780 tgtgcagaga gtaacgcgga gtgtcaagag gtgtgcagaa aatccaaaga aggctgagga 9840 caatgtgtgt gtcaagaaaa taagaaccag aagtcatagg gacagtgaag atatttgaca 9900 gaaaaatcga actgggaaaa atataataaa gttagttttg tgataagttc tagtgcagtt 9960 tttgtcataa attacaagtg aattctgtaa gtaaggctgt cagtctgctt aagggaagaa 10020 aactttggat ttgctgggtc tgaatcggct tcataaactc cactgggagc actgctgggc 10080 tcctggactg agaatagttg aacaccgggg gctttgtgaa ggagtctggg ccaaggtttg 10140 ccctcagctt tgcagaatga agccttgagg tctgtcacca cccacagcca ccctacagca 10200 gccttaactg tgacacttgc cacactgtgt cgtcgtttgt ttgcctatgt cctccagggc 10260 acggtggcag gaacaactat cctcgtctgt cccaacactg agcaggcact cggtaaacac 10320 gaatgaatgg atgagcgcac ggatgaatgg agcttacaga tctgtctttc caatggccgg 10380 ggggatttgg tccccaaatt aaggctattg gacatctgca caggacagtc ta 10432 98 3256 PRT Homo sapiens misc_feature Incyte ID No 2700132CD1 98 Met Trp Pro Thr Arg Arg Leu Val Thr Ile Lys Arg Ser Gly Val 1 5 10 15 Asp Gly Pro His Phe Pro Leu Ser Leu Ser Thr Cys Leu Phe Gly 20 25 30 Arg Gly Ile Glu Cys Asp Ile Arg Ile Gln Leu Pro Val Val Ser 35 40 45 Lys Gln His Cys Lys Ile Glu Ile His Glu Gln Glu Ala Ile Leu 50 55 60 His Asn Phe Ser Ser Thr Asn Pro Thr Gln Val Asn Gly Ser Val 65 70 75 Ile Asp Glu Pro Val Arg Leu Lys His Gly Asp Val Ile Thr Ile 80 85 90 Ile Asp Arg Ser Phe Arg Tyr Glu Asn Glu Ser Leu Gln Ser Gly 95 100 105 Arg Lys Ser Thr Glu Phe Pro Arg Lys Ile Arg Glu Gln Glu Pro 110 115 120 Ala Arg Arg Val Ser Arg Ser Ser Phe Ser Ser Asp Pro Asp Glu 125 130 135 Lys Ala Gln Asp Ser Lys Ala Tyr Ser Lys Ile Thr Glu Gly Lys 140 145 150 Val Ser Gly Asn Pro Gln Val His Ile Lys Asn Val Lys Glu Asp 155 160 165 Ser Thr Ala Asp Asp Ser Lys Asp Ser Val Ala Gln Gly Thr Thr 170 175 180 Asn Val His Ser Ser Glu His Ala Gly Arg Asn Gly Arg Asn Ala 185 190 195 Ala Asp Pro Ile Ser Gly Asp Phe Lys Glu Ile Ser Ser Val Lys 200 205 210 Leu Val Ser Arg Tyr Gly Glu Leu Lys Ser Val Pro Thr Thr Gln 215 220 225 Cys Leu Asp Asn Ser Lys Lys Asn Glu Ser Pro Phe Trp Lys Leu 230 235 240 Tyr Glu Ser Val Lys Lys Glu Leu Asp Val Lys Ser Gln Lys Glu 245 250 255 Asn Val Leu Gln Tyr Cys Arg Lys Ser Gly Leu Gln Thr Asp Tyr 260 265 270 Ala Thr Glu Lys Glu Ser Ala Asp Gly Leu Gln Gly Glu Thr Gln 275 280 285 Leu Leu Val Ser Arg Lys Ser Arg Pro Lys Ser Gly Gly Ser Gly 290 295 300 His Ala Val Ala Glu Pro Ala Ser Pro Glu Gln Glu Leu Asp Gln 305 310 315 Asn Lys Gly Lys Gly Arg Asp Val Glu Ser Val Gln Thr Pro Ser 320 325 330 Lys Ala Val Gly Ala Ser Phe Pro Leu Tyr Glu Pro Ala Lys Met 335 340 345 Lys Thr Pro Val Gln Tyr Ser Gln Gln Gln Asn Ser Pro Gln Lys 350 355 360 His Lys Asn Lys Asp Leu Tyr Thr Thr Gly Arg Arg Glu Ser Val 365 370 375 Asn Leu Gly Lys Ser Glu Gly Phe Lys Ala Gly Asp Lys Thr Leu 380 385 390 Thr Pro Arg Lys Leu Ser Thr Arg Asn Arg Thr Pro Ala Lys Val 395 400 405 Glu Asp Ala Ala Asp Ser Ala Thr Lys Pro Glu Asn Leu Ser Ser 410 415 420 Lys Thr Arg Gly Ser Ile Pro Thr Asp Val Glu Val Leu Pro Thr 425 430 435 Glu Thr Glu Ile His Asn Glu Pro Phe Leu Thr Leu Trp Leu Thr 440 445 450 Gln Val Glu Arg Lys Ile Gln Lys Asp Ser Leu Ser Lys Pro Glu 455 460 465 Lys Leu Gly Thr Thr Ala Gly Gln Met Cys Ser Gly Leu Pro Gly 470 475 480 Leu Ser Ser Val Asp Ile Asn Asn Phe Gly Asp Ser Ile Asn Glu 485 490 495 Ser Glu Gly Ile Pro Leu Lys Arg Arg Arg Val Ser Phe Gly Gly 500 505 510 His Leu Arg Pro Glu Leu Phe Asp Glu Asn Leu Pro Pro Asn Thr 515 520 525 Pro Leu Lys Arg Gly Glu Ala Pro Thr Lys Arg Lys Ser Leu Val 530 535 540 Met His Thr Pro Pro Val Leu Lys Lys Ile Ile Lys Glu Gln Pro 545 550 555 Gln Pro Ser Gly Lys Gln Glu Ser Gly Ser Glu Ile His Val Glu 560 565 570 Val Lys Ala Gln Ser Leu Val Ile Ser Pro Pro Ala Pro Ser Pro 575 580 585 Arg Lys Thr Pro Val Ala Ser Asp Gln Arg Arg Arg Ser Cys Lys 590 595 600 Thr Ala Pro Ala Ser Ser Ser Lys Ser Gln Thr Glu Val Pro Lys 605 610 615 Arg Gly Gly Glu Arg Val Ala Thr Cys Leu Gln Lys Arg Val Ser 620 625 630 Ile Ser Arg Ser Gln His Asp Ile Leu Gln Met Ile Cys Ser Lys 635 640 645 Arg Arg Ser Gly Ala Ser Glu Ala Asn Leu Ile Val Ala Lys Ser 650 655 660 Trp Ala Asp Val Val Lys Leu Gly Ala Lys Gln Thr Gln Thr Lys 665 670 675 Val Ile Lys His Gly Pro Gln Arg Ser Met Asn Lys Arg Gln Arg 680 685 690 Arg Pro Ala Thr Pro Lys Lys Pro Val Gly Glu Val His Ser Gln 695 700 705 Phe Ser Thr Gly His Ala Asn Ser Pro Cys Thr Ile Ile Ile Gly 710 715 720 Lys Ala His Thr Glu Lys Val His Val Pro Ala Arg Pro Tyr Arg 725 730 735 Val Leu Asn Asn Phe Ile Ser Asn Gln Lys Met Asp Phe Lys Glu 740 745 750 Asp Leu Ser Gly Ile Ala Glu Met Phe Lys Thr Pro Val Lys Glu 755 760 765 Gln Pro Gln Leu Thr Ser Thr Cys His Ile Ala Ile Ser Asn Ser 770 775 780 Glu Asn Leu Leu Gly Lys Gln Phe Gln Gly Thr Asp Ser Gly Glu 785 790 795 Glu Pro Leu Leu Pro Thr Ser Glu Ser Phe Gly Gly Asn Val Phe 800 805 810 Phe Ser Ala Gln Asn Ala Ala Lys Gln Pro Ser Asp Lys Cys Ser 815 820 825 Ala Ser Pro Pro Leu Arg Arg Gln Cys Ile Arg Glu Asn Gly Asn 830 835 840 Val Ala Lys Thr Pro Arg Asn Thr Tyr Lys Met Thr Ser Leu Glu 845 850 855 Thr Lys Thr Ser Asp Thr Glu Thr Glu Pro Ser Lys Thr Val Ser 860 865 870 Thr Val Asn Arg Ser Gly Arg Ser Thr Glu Phe Arg Asn Ile Gln 875 880 885 Lys Leu Pro Val Glu Ser Lys Ser Glu Glu Thr Asn Thr Glu Ile 890 895 900 Val Glu Cys Ile Leu Lys Arg Gly Gln Lys Ala Thr Leu Leu Gln 905 910 915 Gln Arg Arg Glu Gly Glu Met Lys Glu Ile Glu Arg Pro Phe Glu 920 925 930 Thr Tyr Lys Glu Asn Ile Glu Leu Lys Glu Asn Asp Glu Lys Met 935 940 945 Lys Ala Met Lys Arg Ser Arg Thr Trp Gly Gln Lys Cys Ala Pro 950 955 960 Met Ser Asp Leu Thr Asp Leu Lys Ser Leu Pro Asp Thr Glu Leu 965 970 975 Met Lys Asp Thr Ala Arg Gly Gln Asn Leu Leu Gln Thr Gln Asp 980 985 990 His Ala Lys Ala Pro Lys Ser Glu Lys Gly Lys Ile Thr Lys Met 995 1000 1005 Pro Cys Gln Ser Leu Gln Pro Glu Pro Ile Asn Thr Pro Thr His 1010 1015 1020 Thr Lys Gln Gln Leu Lys Ala Ser Leu Gly Lys Val Gly Val Lys 1025 1030 1035 Glu Glu Leu Leu Ala Val Gly Lys Phe Thr Arg Thr Ser Gly Glu 1040 1045 1050 Thr Thr His Thr His Arg Glu Pro Ala Gly Asp Gly Lys Ser Ile 1055 1060 1065 Arg Thr Phe Lys Glu Ser Pro Lys Gln Ile Leu Asp Pro Ala Ala 1070 1075 1080 Arg Val Thr Gly Met Lys Lys Trp Pro Arg Thr Pro Lys Glu Glu 1085 1090 1095 Ala Gln Ser Leu Glu Asp Leu Ala Gly Phe Lys Glu Leu Phe Gln 1100 1105 1110 Thr Pro Gly Pro Ser Glu Glu Ser Met Thr Asp Glu Lys Thr Thr 1115 1120 1125 Lys Ile Ala Cys Lys Ser Pro Pro Pro Glu Ser Val Asp Thr Pro 1130 1135 1140 Thr Ser Thr Lys Gln Trp Pro Lys Arg Ser Leu Arg Lys Ala Asp 1145 1150 1155 Val Glu Glu Glu Phe Leu Ala Leu Arg Lys Leu Thr Pro Ser Ala 1160 1165 1170 Gly Lys Ala Met Leu Thr Pro Lys Pro Ala Gly Gly Asp Glu Lys 1175 1180 1185 Asp Ile Lys Ala Phe Met Gly Thr Pro Val Gln Lys Leu Asp Leu 1190 1195 1200 Ala Gly Thr Leu Pro Gly Ser Lys Arg Gln Leu Gln Thr Pro Lys 1205 1210 1215 Glu Lys Ala Gln Ala Leu Glu Asp Leu Ala Gly Phe Lys Glu Leu 1220 1225 1230 Phe Gln Thr Pro Gly His Thr Glu Glu Leu Val Ala Ala Gly Lys 1235 1240 1245 Thr Thr Lys Ile Pro Cys Asp Ser Pro Gln Ser Asp Pro Val Asp 1250 1255 1260 Thr Pro Thr Ser Thr Lys Gln Arg Pro Lys Arg Ser Ile Arg Lys 1265 1270 1275 Ala Asp Val Glu Gly Glu Leu Leu Ala Cys Arg Asn Leu Met Pro 1280 1285 1290 Ser Ala Gly Lys Ala Met His Thr Pro Lys Pro Ser Val Gly Glu 1295 1300 1305 Glu Lys Asp Ile Ile Ile Phe Val Gly Thr Pro Val Gln Lys Leu 1310 1315 1320 Asp Leu Thr Glu Asn Leu Thr Gly Ser Lys Arg Arg Pro Gln Thr 1325 1330 1335 Pro Lys Glu Glu Ala Gln Ala Leu Glu Asp Leu Thr Gly Phe Lys 1340 1345 1350 Glu Leu Phe Gln Thr Pro Gly His Thr Glu Glu Ala Val Ala Ala 1355 1360 1365 Gly Lys Thr Thr Lys Met Pro Cys Glu Ser Ser Pro Pro Glu Ser 1370 1375 1380 Ala Asp Thr Pro Thr Ser Thr Arg Arg Gln Pro Lys Thr Pro Leu 1385 1390 1395 Glu Lys Arg Asp Val Gln Lys Glu Leu Ser Ala Leu Lys Lys Leu 1400 1405 1410 Thr Gln Thr Ser Gly Glu Thr Thr His Thr Asp Lys Val Pro Gly 1415 1420 1425 Gly Glu Asp Lys Ser Ile Asn Ala Phe Arg Glu Thr Ala Lys Gln 1430 1435 1440 Lys Leu Asp Pro Ala Ala Ser Val Thr Gly Ser Lys Arg His Pro 1445 1450 1455 Lys Thr Lys Glu Lys Ala Gln Pro Leu Glu Asp Leu Ala Gly Trp 1460 1465 1470 Lys Glu Leu Phe Gln Thr Pro Val Cys Thr Asp Lys Pro Thr Thr 1475 1480 1485 His Glu Lys Thr Thr Lys Ile Ala Cys Arg Ser Gln Pro Asp Pro 1490 1495 1500 Val Asp Thr Pro Thr Ser Ser Lys Pro Gln Ser Lys Arg Ser Leu 1505 1510 1515 Arg Lys Val Asp Val Glu Glu Glu Phe Phe Ala Leu Arg Lys Arg 1520 1525 1530 Thr Pro Ser Ala Gly Lys Ala Met His Thr Pro Lys Pro Ala Val 1535 1540 1545 Ser Gly Glu Lys Asn Ile Tyr Ala Phe Met Gly Thr Pro Val Gln 1550 1555 1560 Lys Leu Asp Leu Thr Glu Asn Leu Thr Gly Ser Lys Arg Arg Leu 1565 1570 1575 Gln Thr Pro Lys Glu Lys Ala Gln Ala Leu Glu Asp Leu Ala Gly 1580 1585 1590 Phe Lys Glu Leu Phe Gln Thr Arg Gly His Thr Glu Glu Ser Met 1595 1600 1605 Thr Asn Asp Lys Thr Ala Lys Val Ala Cys Lys Ser Ser Gln Pro 1610 1615 1620 Asp Leu Asp Lys Asn Pro Ala Ser Ser Lys Arg Arg Leu Lys Thr 1625 1630 1635 Ser Leu Gly Lys Val Gly Val Lys Glu Glu Leu Leu Ala Val Gly 1640 1645 1650 Lys Leu Thr Gln Thr Ser Gly Glu Thr Thr His Thr His Thr Glu 1655 1660 1665 Pro Thr Gly Asp Gly Lys Ser Met Lys Ala Phe Met Glu Ser Pro 1670 1675 1680 Lys Gln Ile Leu Asp Ser Ala Ala Ser Leu Thr Gly Ser Lys Arg 1685 1690 1695 Gln Leu Arg Thr Pro Lys Gly Lys Ser Glu Val Pro Glu Asp Leu 1700 1705 1710 Ala Gly Phe Ile Glu Leu Phe Gln Thr Pro Ser His Thr Lys Glu 1715 1720 1725 Ser Met Thr Asn Glu Lys Thr Thr Lys Val Ser Tyr Arg Ala Ser 1730 1735 1740 Gln Pro Asp Leu Val Asp Thr Pro Thr Ser Ser Lys Pro Gln Pro 1745 1750 1755 Lys Arg Ser Leu Arg Lys Ala Asp Thr Glu Glu Glu Phe Leu Ala 1760 1765 1770 Phe Arg Lys Gln Thr Pro Ser Ala Gly Lys Ala Met His Thr Pro 1775 1780 1785 Lys Pro Ala Val Gly Glu Glu Lys Asp Ile Asn Thr Phe Leu Gly 1790 1795 1800 Thr Pro Val Gln Lys Leu Asp Gln Pro Gly Asn Leu Pro Gly Ser 1805 1810 1815 Asn Arg Arg Leu Gln Thr Arg Lys Glu Lys Ala Gln Ala Leu Glu 1820 1825 1830 Glu Leu Thr Gly Phe Arg Glu Leu Phe Gln Thr Pro Cys Thr Asp 1835 1840 1845 Asn Pro Thr Thr Asp Glu Lys Thr Thr Lys Lys Ile Leu Cys Lys 1850 1855 1860 Ser Pro Gln Ser Asp Pro Ala Asp Thr Pro Thr Asn Thr Lys Gln 1865 1870 1875 Arg Pro Lys Arg Ser Leu Lys Lys Ala Asp Val Glu Glu Glu Phe 1880 1885 1890 Leu Ala Phe Arg Lys Leu Thr Pro Ser Ala Gly Lys Ala Met His 1895 1900 1905 Thr Pro Lys Ala Ala Val Gly Glu Glu Lys Asp Ile Asn Thr Phe 1910 1915 1920 Val Gly Thr Pro Val Glu Lys Leu Asp Leu Leu Gly Asn Leu Pro 1925 1930 1935 Gly Ser Lys Arg Arg Pro Gln Thr Pro Lys Glu Lys Ala Lys Ala 1940 1945 1950 Leu Glu Asp Leu Ala Gly Phe Lys Glu Leu Phe Gln Thr Pro Gly 1955 1960 1965 His Thr Glu Glu Ser Met Thr Asp Asp Lys Ile Thr Glu Val Ser 1970 1975 1980 Cys Lys Ser Pro Gln Pro Asp Pro Val Lys Thr Pro Thr Ser Ser 1985 1990 1995 Lys Gln Arg Leu Lys Ile Ser Leu Gly Lys Val Gly Val Lys Glu 2000 2005 2010 Glu Val Leu Pro Val Gly Lys Leu Thr Gln Thr Ser Gly Lys Thr 2015 2020 2025 Thr Gln Thr His Arg Glu Thr Ala Gly Asp Gly Lys Ser Ile Lys 2030 2035 2040 Ala Phe Lys Glu Ser Ala Lys Gln Met Leu Asp Pro Ala Asn Tyr 2045 2050 2055 Gly Thr Gly Met Glu Arg Trp Pro Arg Thr Pro Lys Glu Glu Ala 2060 2065 2070 Gln Ser Leu Glu Asp Leu Ala Gly Phe Lys Glu Leu Phe Gln Thr 2075 2080 2085 Pro Asp His Thr Glu Glu Ser Thr Thr Asp Asp Lys Thr Thr Lys 2090 2095 2100 Ile Ala Cys Lys Ser Pro Pro Pro Glu Ser Met Asp Thr Pro Thr 2105 2110 2115 Ser Thr Arg Arg Arg Pro Lys Thr Pro Leu Gly Lys Arg Asp Ile 2120 2125 2130 Val Glu Glu Leu Ser Ala Leu Lys Gln Leu Thr Gln Thr Thr His 2135 2140 2145 Thr Asp Lys Val Pro Gly Asp Glu Asp Lys Gly Ile Asn Val Phe 2150 2155 2160 Arg Glu Thr Ala Lys Gln Lys Leu Asp Pro Ala Ala Ser Val Thr 2165 2170 2175 Gly Ser Lys Arg Gln Pro Arg Thr Pro Lys Gly Lys Ala Gln Pro 2180 2185 2190 Leu Glu Asp Leu Ala Gly Leu Lys Glu Leu Phe Gln Thr Pro Ile 2195 2200 2205 Cys Thr Asp Lys Pro Thr Thr His Glu Lys Thr Thr Lys Ile Ala 2210 2215 2220 Cys Arg Ser Pro Gln Pro Asp Pro Val Gly Thr Pro Thr Ile Phe 2225 2230 2235 Lys Pro Gln Ser Lys Arg Ser Leu Arg Lys Ala Asp Val Glu Glu 2240 2245 2250 Glu Ser Leu Ala Leu Arg Lys Arg Thr Pro Ser Val Gly Lys Ala 2255 2260 2265 Met Asp Thr Pro Lys Pro Ala Gly Gly Asp Glu Lys Asp Met Lys 2270 2275 2280 Ala Phe Met Gly Thr Pro Val Gln Lys Leu Asp Leu Pro Gly Asn 2285 2290 2295 Leu Pro Gly Ser Lys Arg Trp Pro Gln Thr Pro Lys Glu Lys Ala 2300 2305 2310 Gln Ala Leu Glu Asp Leu Ala Gly Phe Lys Glu Leu Phe Gln Thr 2315 2320 2325 Pro Gly Thr Asp Lys Pro Thr Thr Asp Glu Lys Thr Thr Lys Ile 2330 2335 2340 Ala Cys Lys Ser Pro Gln Pro Asp Pro Val Asp Thr Pro Ala Ser 2345 2350 2355 Thr Lys Gln Arg Pro Lys Arg Asn Leu Arg Lys Ala Asp Val Glu 2360 2365 2370 Glu Glu Phe Leu Ala Leu Arg Lys Arg Thr Pro Ser Ala Gly Lys 2375 2380 2385 Ala Met Asp Thr Pro Lys Pro Ala Val Ser Asp Glu Lys Asn Ile 2390 2395 2400 Asn Thr Phe Val Glu Thr Pro Val Gln Lys Leu Asp Leu Leu Gly 2405 2410 2415 Asn Leu Pro Gly Ser Lys Arg Gln Pro Gln Thr Pro Lys Glu Lys 2420 2425 2430 Ala Glu Ala Leu Glu Asp Leu Val Gly Phe Lys Glu Leu Phe Gln 2435 2440 2445 Thr Pro Gly His Thr Glu Glu Ser Met Thr Asp Asp Lys Ile Thr 2450 2455 2460 Glu Val Ser Cys Lys Ser Pro Gln Pro Glu Ser Phe Lys Thr Ser 2465 2470 2475 Arg Ser Ser Lys Gln Arg Leu Lys Ile Pro Leu Val Lys Val Asp 2480 2485 2490 Met Lys Glu Glu Pro Leu Ala Val Ser Lys Leu Thr Arg Thr Ser 2495 2500 2505 Gly Glu Thr Thr Gln Thr His Thr Glu Pro Thr Gly Asp Ser Lys 2510 2515 2520 Ser Ile Lys Ala Phe Lys Glu Ser Pro Lys Gln Ile Leu Asp Pro 2525 2530 2535 Ala Ala Ser Val Thr Gly Ser Arg Arg Gln Leu Arg Thr Arg Lys 2540 2545 2550 Glu Lys Ala Arg Ala Leu Glu Asp Leu Val Asp Phe Lys Glu Leu 2555 2560 2565 Phe Ser Ala Pro Gly His Thr Glu Glu Ser Met Thr Ile Asp Lys 2570 2575 2580 Asn Thr Lys Ile Pro Cys Lys Ser Pro Pro Pro Glu Leu Thr Asp 2585 2590 2595 Thr Ala Thr Ser Thr Lys Arg Cys Pro Lys Thr Arg Leu Arg Lys 2600 2605 2610 Glu Val Lys Glu Glu Leu Ser Ala Val Glu Arg Leu Thr Gln Thr 2615 2620 2625 Ser Gly Gln Ser Thr His Thr His Lys Glu Pro Ala Ser Gly Asp 2630 2635 2640 Glu Gly Ile Lys Val Leu Lys Gln Arg Ala Lys Lys Lys Pro Asn 2645 2650 2655 Pro Val Glu Glu Glu Pro Ser Arg Arg Arg Pro Arg Ala Pro Lys 2660 2665 2670 Glu Lys Ala Gln Pro Leu Glu Asp Leu Ala Gly Phe Thr Glu Leu 2675 2680 2685 Ser Glu Thr Ser Gly His Thr Gln Glu Ser Leu Thr Ala Gly Lys 2690 2695 2700 Ala Thr Lys Ile Pro Cys Glu Ser Pro Pro Leu Glu Val Val Asp 2705 2710 2715 Thr Thr Ala Ser Thr Lys Arg His Leu Arg Thr Arg Val Gln Lys 2720 2725 2730 Val Gln Val Lys Glu Glu Pro Ser Ala Val Lys Phe Thr Gln Thr 2735 2740 2745 Ser Gly Glu Thr Thr Asp Ala Asp Lys Glu Pro Ala Gly Glu Asp 2750 2755 2760 Lys Gly Ile Lys Ala Leu Lys Glu Ser Ala Lys Gln Thr Pro Ala 2765 2770 2775 Pro Ala Ala Ser Val Thr Gly Ser Arg Arg Arg Pro Arg Ala Pro 2780 2785 2790 Arg Glu Ser Ala Gln Ala Ile Glu Asp Leu Ala Gly Phe Lys Asp 2795 2800 2805 Pro Ala Ala Gly His Thr Glu Glu Ser Met Thr Asp Asp Lys Thr 2810 2815 2820 Thr Lys Ile Pro Cys Lys Ser Ser Pro Glu Leu Glu Asp Thr Ala 2825 2830 2835 Thr Ser Ser Lys Arg Arg Pro Arg Thr Arg Ala Gln Lys Val Glu 2840 2845 2850 Val Lys Glu Glu Leu Leu Ala Val Gly Lys Leu Thr Gln Thr Ser 2855 2860 2865 Gly Glu Thr Thr His Thr Asp Lys Glu Pro Val Gly Glu Gly Lys 2870 2875 2880 Gly Thr Lys Ala Phe Lys Gln Pro Ala Lys Arg Lys Leu Asp Ala 2885 2890 2895 Glu Asp Val Ile Gly Ser Arg Arg Gln Pro Arg Ala Pro Lys Glu 2900 2905 2910 Lys Ala Gln Pro Leu Glu Asp Leu Ala Ser Phe Gln Glu Leu Ser 2915 2920 2925 Gln Thr Pro Gly His Thr Glu Glu Leu Ala Asn Gly Ala Ala Asp 2930 2935 2940 Ser Phe Thr Ser Ala Pro Lys Gln Thr Pro Asp Ser Gly Lys Pro 2945 2950 2955 Leu Lys Ile Ser Arg Arg Val Leu Arg Ala Pro Lys Val Glu Pro 2960 2965 2970 Val Gly Asp Val Val Ser Thr Arg Asp Pro Val Lys Ser Gln Ser 2975 2980 2985 Lys Ser Asn Thr Ser Leu Pro Pro Leu Pro Phe Lys Arg Gly Gly 2990 2995 3000 Gly Lys Asp Gly Ser Val Thr Gly Thr Lys Arg Leu Arg Cys Met 3005 3010 3015 Pro Ala Pro Glu Glu Ile Val Glu Glu Leu Pro Ala Ser Lys Lys 3020 3025 3030 Gln Arg Val Ala Pro Arg Ala Arg Gly Lys Ser Ser Glu Pro Val 3035 3040 3045 Val Ile Met Lys Arg Ser Leu Arg Thr Ser Ala Lys Arg Ile Glu 3050 3055 3060 Pro Ala Glu Glu Leu Asn Ser Asn Asp Met Lys Thr Asn Lys Glu 3065 3070 3075 Glu His Lys Leu Gln Asp Ser Val Pro Glu Asn Lys Gly Ile Ser 3080 3085 3090 Leu Arg Ser Arg Arg Gln Asn Lys Thr Glu Ala Glu Gln Gln Ile 3095 3100 3105 Thr Glu Val Phe Val Leu Ala Glu Arg Ile Glu Ile Asn Arg Asn 3110 3115 3120 Glu Lys Lys Pro Met Lys Thr Ser Pro Glu Met Asp Ile Gln Asn 3125 3130 3135 Pro Asp Asp Gly Ala Arg Lys Pro Ile Pro Arg Asp Lys Val Thr 3140 3145 3150 Glu Asn Lys Arg Cys Leu Arg Ser Ala Arg Gln Asn Glu Ser Ser 3155 3160 3165 Gln Pro Lys Val Ala Glu Glu Ser Gly Gly Gln Lys Ser Ala Lys 3170 3175 3180 Val Leu Met Gln Asn Gln Lys Gly Lys Gly Glu Ala Gly Asn Ser 3185 3190 3195 Asp Ser Met Cys Leu Arg Ser Arg Lys Thr Lys Ser Gln Pro Ala 3200 3205 3210 Ala Ser Thr Leu Glu Ser Lys Ser Val Gln Arg Val Thr Arg Ser 3215 3220 3225 Val Lys Arg Cys Ala Glu Asn Pro Lys Lys Ala Glu Asp Asn Val 3230 3235 3240 Cys Val Lys Lys Ile Arg Thr Arg Ser His Arg Asp Ser Glu Asp 3245 3250 3255 Ile 99 826 DNA Homo sapiens misc_feature Incyte ID No 211881.1 99 cttaaaacct gacatccttc atgttagcta acctttataa tctctttgga tgtagtaaat 60 ttttagtatt ttttagattg aatttgtatc atatttgcta gcaaattgag tataaagagt 120 agcatatttt tactacagat gtattatttt aactaacaaa ggcatattat acattttttt 180 catatataaa ctttggaata ggattttaca gtaacttaag ttttttattt ctacccatgt 240 gtcaaagttt tatgctaaat tctgaataga atagttgtaa ctcccactct gggtatttta 300 tttattttaa acagttctag tattgtttcc tgtgaatttt ttccagggat tgctactttc 360 tgcactattc attagaccaa gagcatttca ccaaatactt aaaacttaaa aatttttaaa 420 cttttccaaa tttgattaaa aggataacat attctaaagg tattcaatat ttttacttat 480 ctctgaaaaa cttaatcaca taaaagcata cattttacac atacagctct ctccatcttc 540 cacaatagat taagacataa aacataacca gtatttttga aaagccccct taactggcat 600 gcttcttact gaaattatca taaaaggttc gtatgagaaa ggattccaga atatccctta 660 attgtgttgt agcttatgca tttctattta ttttatacat tatttaattc atgtgagtta 720 cttacctggc agggaagata tgatcaccaa ggtgcctttc acattcattg cactctggat 780 gtgctgaccc ctgcaatttc cccaaatggg ggaagctcaa ctgcat 826 100 1498 DNA Homo sapiens misc_feature Incyte ID No 409895.2 100 agctaatgtg ttacattaga atcacctcgg ggaggccctg ggtgcccttc tcagccctcc 60 ctccggaggc tgctgaagcc cagcaaagcc ggagtcagag aacaatgtcc gcctgagggc 120 agggctgggc tgggctggcc ttctggccct atctgctccg tgcccaaccc agcgccccgc 180 acagtcggag ctttgtaaat acgaggtgac tgtctgccta caaactttgt aaacatcact 240 tgaaatggcc gcagggtatt gcgacatggc cataccacta tttgtttgct attgaatttg 300 tacttccctg ccttactttt gctattgcaa accatgctgt cactaaggtc ttcatgcaca 360 cagttgtgtc ttggtcagat gatatgtttc taccaatttt aattgtgttt ctttccacct 420 gggacacaca gctctctggg ccccagggct gggtcatcag cacaccctgc tgctgctgtt 480 cagatctgca tcctggtccc gcttggtccc acagtgagaa cgctttgcta tcacatgggc 540 aggctctgag agccctgccg gcctggcctt ctcaaagaag acctgagagc ttgggaccca 600 agcagagagg aagaacaggg ctcagggtgc ttgctccatg ctcgctccac acctggggct 660 caaccctggc tttccccggc tccctgtgtg acttcagggc aggtcccttg ggccctctgg 720 gccttatcat cttcatctgt aacagggcga tgcctctgcc gtgtctggtg gtgttgagga 780 gttcctgttt gtgtaagcag ctagttcagt gccagcacga gatgggaggc ccatgaagtt 840 agcagtgcac aaaaaataga gcaaagactg gatgcatttc ctgagaacaa ccatcactgt 900 aaagcacttt acaaatccaa agacaacccc cggcaaaaac tcaaaatgaa actccctctc 960 gcagagcaca attccaattc gctctaaaaa cattacaagt tagttcatgt catgccagat 1020 agctgaaggc agctcacaag ttcttaaggc caggaatgcc atgtgtctgc tatgcacagc 1080 tggccctggc cctgagcctg aatgacagca aaggtgacgc agatgtgggt gccctgctcc 1140 tgcccagcag cagtgcttgg tggaggctga ggccctgcac aggcaccctc actgctgacc 1200 ttgagcctct ctctcctcta gagtggaaaa gacaaggatg ccgtggataa attgctcaag 1260 gacctggacg ccaatggaga tgcccaggtg gacttcagtg agttcatcgt gttcgtggct 1320 gcaatcacgt ctgcctgtca caagtacttt gagaaggcag gactcaaatg atgccctgga 1380 gatgtcacag attcctggca gagccatggt cccaggcttc ccaaaagtgt ttgttggcaa 1440 ttattcccct aggctgagcc tgctcatgta cctctgatta ataaatgctt atgaaatg 1498 101 860 DNA Homo sapiens misc_feature Incyte ID No 1422432CB1 101 agagcaaaga ctggatgcat ttcctgagaa caaccatcac tgtaaagcac tttacaaatc 60 caaagacaac ccccggcaaa aactcaaaat gaaactccct ctcgcagagc acaattccaa 120 ttcgctctaa aaacattaca agttagttca tgtcatgcca gatagctgaa ggcagctcac 180 aagttcttaa ggccaggaat gccangtgtc tgctatgcac agctggccct ggccctgagc 240 ctgaatgaca gcaaaggtga cgcagatgtg ggtgccctgc tcctgcccag cagcagtgct 300 tggtggaggc tgaggccctg cacaggcacc ctcactgctg accttgagcc tctctctcct 360 ctcaagaggc tgccagtggg acattttctc ggccctgcca gcccccagga ggaaggtggg 420 tctgaatcta gcaccatgac ggaactagag acagccatgg gcatgatcat agacgtcttt 480 tcccgatatt cgggcagcga gggcagcacg cagaccctga ccaaggggga gctcaaggtg 540 ctgatggaga aggagctacc aggcttcctg cagagtggaa aagacaagga tgccgtggat 600 aaattgctca aggacctgga cgccaatgga gatgcccagg tggacttcag tgagttcatc 660 gtgttcgtgg ctgcaatcac gtctgcctgt cacaagtact ttgagaaggc aggactcaaa 720 tgatgccctg gagatgtcac agattcctgg cagagccatg gtcccaggct tcccaaaagt 780 gtttgttggc aattattccc ctaggctgag cctgctcatg tacctctgat taataaatgc 840 ttatgaaatg aaaaaaaaaa 860 102 95 PRT Homo sapiens misc_feature Incyte ID No 1422432CD1 102 Met Thr Glu Leu Glu Thr Ala Met Gly Met Ile Ile Asp Val Phe 1 5 10 15 Ser Arg Tyr Ser Gly Ser Glu Gly Ser Thr Gln Thr Leu Thr Lys 20 25 30 Gly Glu Leu Lys Val Leu Met Glu Lys Glu Leu Pro Gly Phe Leu 35 40 45 Gln Ser Gly Lys Asp Lys Asp Ala Val Asp Lys Leu Leu Lys Asp 50 55 60 Leu Asp Ala Asn Gly Asp Ala Gln Val Asp Phe Ser Glu Phe Ile 65 70 75 Val Phe Val Ala Ala Ile Thr Ser Ala Cys His Lys Tyr Phe Glu 80 85 90 Lys Ala Gly Leu Lys 95 

What is claimed is:
 1. A composition comprising a plurality of cDNAs that are differentially expressed in prostate cancer and selected from SEQ ID NOs:1-3, 5, 6, 8, 10-15, 17-19, 21, 23-28, 30, 32, 34-36, 38, 40, 42-45, 47-50, 52, 53, 55, 56, 58-65, 67, 68, 70-73, 75, 76, 78-86, 88-90, 92-97, 99-101 or their complements.
 2. The composition of claim 1, wherein each of the cDNAs is differentially regulated between non-metastatic and metastatic prostate cancer and is selected from SEQ ID NOs:1-3, 5, 6, 8, 10-15, 17-19, 21, 23-28, 30, 32, 34-36, 38, 40, 42-45, 47-50, 52, 53, 55, 56, 58-65, 67, 68, 70-73,
 75. 3. The composition of claim 1, wherein each of the cDNAs is differentially regulated between prostate cancer and normal prostate and is selected from SEQ ID NOs:76, 78-86, 88-90, 92-97, 99-101.
 4. The composition of claim 1, wherein the cDNAs are immobilized on a substrate.
 5. A high throughput method for detecting differential expression of one or more cDNAs in a sample containing nucleic acids, the method comprising: (a) hybridizing the substrate of claim 4 with nucleic acids of the sample, thereby fomming one or more hybridization complexes; (b) detecting the hybridization complexes; and (c) comparing the hybridization complexes with those of a standard, wherein differences between the standard and sample hybridization complexes indicate differential expression of cDNAs in the sample.
 6. The method of claim 5, wherein the nucleic acids of the sample are amplified prior to hybridization.
 7. The method of claim 5, wherein the sample is from a subject with prostate cancer and comparison with a standard defines an early, mid, or late stage of that disease.
 8. A high throughput method of screening a plurality of molecules or compounds to identify a ligand which specifically binds a cDNA, the method comprising: (a) combining the composition of claim 1 with the plurality of molecules or compounds under conditions to allow specific binding; and (b) detecting specific binding between each cDNA and at least one molecule or compound, thereby identifying a ligand that specifically binds to each cDNA.
 9. The method of claim 8 wherein the plurality of molecules or compounds are selected from DNA molecules, RNA molecules, peptide nucleic acid molecules, mimetics, peptides, transcription factors, repressors, and regulatory proteins.
 10. An isolated cDNA encoding a protein comprising the amino acid sequence of SEQ ID NO:36.
 11. A vector containing the cDNA of claim
 10. 12. A host cell containing the vector of claim
 11. 13. A method for producing a protein, the method comprising the steps of: (a) culturing the host cell of claim 12 under conditions for expression of protein; and (b) recovering the protein from the host cell culture.
 14. A protein or a portion thereof produced by the method of claim
 13. 15. A high-throughput method for using a protein to screen a plurality of molecules or compounds to identify at least one ligand which specifically binds the protein, the method comprising: (a) combining the protein of claim 14 with the plurality of molecules or compounds under conditions to allow specific binding; and (b) detecting specific binding between the protein and a molecule or compound, thereby identifying a ligand which specifically binds the protein.
 16. The method of claim 15 wherein the plurality of molecules or compounds is selected from DNA molecules, RNA molecules, peptide nucleic acid molecules, mimetics, peptides, proteins, agonists, antagonists, antibodies or their fragments, immunoglobulins, inhibitors, drug compounds, and pharmaceutical agents.
 17. A method of using a protein to produce an antibody, the method comprising: a) immunizing an animal with the protein of claim 14 under conditions to elicit an antibody response; b) isolating animal antibodies; and c) screening the isolated antibodies with the protein, thereby identifying an antibody which specifically binds the protein.
 18. A method of purifying an antibody, the method comprising: a) combining the protein of claim 14 with a sample under conditions to allow specific binding; b) recovering the bound protein; and c) separating the protein from the antibody, thereby obtaining purified antibody. 